TW202045469A - 用於治療肺纖維化、肝纖維化、皮膚纖維化及心臟纖維化之經取代之芳族化合物 - Google Patents
用於治療肺纖維化、肝纖維化、皮膚纖維化及心臟纖維化之經取代之芳族化合物 Download PDFInfo
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Abstract
本發明係關於用於預防或治療個體之各種纖維變性疾病及病狀,包括肺纖維化、肝纖維化、皮膚纖維化及心臟纖維化的經取代之芳族化合物,其中該化合物具有下式:
或其醫藥學上可接受之鹽,其中
A為C5烷基、C6烷基、C5烯基、C6烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為3或4;
R1為H、OH或F;
R2為H、OH、F或CH2-OH;
R3為H、OH、F或CH2Ph;
R4為H、OH或F;
Q為
1)(CH2)mC(O)OH,其中m為1或2,
2)CH(CH3)C(O)OH,
3)C(CH3)2C(O)OH,
4)CH(F)-C(O)OH,
5)CF2-C(O)OH,或
6)C(O)-C(O)OH。
Description
本發明係關於經取代之芳族化合物、其製備、包含其之組成物以及其用於預防或治療個體之各種纖維變性疾病及病狀,包括肺纖維化、肝纖維化、皮膚纖維化及心臟纖維化的用途。
肺纖維化
肺纖維化(lung fibrosis/pulmonaryfibrosis)為一種涉及肺組織瘢痕形成之嚴重醫學病狀。當肺泡及肺間質組織發炎且在組織上形成瘢痕以試圖自我修復時,出現此病狀。肺纖維化涉及正常肺實質與纖維變性組織(纖維瘢痕)之逐漸交換。正常之肺經瘢痕組織置換造成氧擴散能力不可逆地下降。目前,尚未有可逆轉肺組織之此瘢痕形成的治療措施或手段。
可以造成肺纖維化之許多病狀包括慢性發炎過程(肉狀瘤病、韋格納氏肉芽腫病(Wegener's granulomatosis))、感染、環境劑(石棉、二氧化矽、暴露於某些氣體)、曝露於電離輻射(諸如治療胸部腫瘤之輻射療法)、慢性病狀(狼瘡),以及某些藥物治療(例如胺碘酮(amiodarone)、博萊黴素(bleomycin)、平陽黴素(pingyangmycin)、白消安(busulfan)、甲胺喋呤(methotrexate)及呋喃妥因(nitrofurantoin))。
在稱為過敏性肺炎之病狀中,針對吸入有機粉塵或職業化學物質之免疫反應提高後可形成肺之纖維化。此病狀最通常起因於吸入受細
菌、真菌或動物產品污染之粉塵。
COPD(慢性阻塞性肺病)為肺纖維化之另一形式(Gosker 等人,(2003)「Myopathological features in skeletal muscle of patients with chronic obstructive pulmonary disease」Eur.Respir.J.22(2),280-285),其由對肺組織之煙霧刺激造成。吸煙為COPD之最常見原因,而多種其他因素諸如空氣污染及遺傳學起到較小作用。在開發中世界,空氣污染之常見來源之一為烹飪及取暖用火之通風不良。長期暴露於此等刺激物會造成肺中出現發炎反應,導致小氣管狹窄及肺組織破壞,此稱為肺氣腫。診斷係基於藉由肺功能測試所量測之氣流不暢。與哮喘不同,藉由投予目前批准之藥物治療不會顯著改善氣流減少。可藉由減少暴露於已知原因來預防COPD。此包括努力降低吸煙率及改善室內及室外空氣品質。COPD治療包括:戒煙、疫苗接種、改變生活習慣及通常吸入支氣管擴張劑及類固醇類。有些人可自長期氧療法或肺移植獲益。在具有急性惡化期之患者中,可能需要增加藥物使用及住院治療。
囊腫性纖維化(CF)亦為肺纖維化之另一形式。CF為一種常染色體隱性遺傳性病症,其在臨床上最常影響肺、以及胰臟、肝臟及腸。其特徵在於氯離子及鈉跨越上皮之輸送異常,導致粘稠分泌物。名稱囊腫性纖維化係指胰臟內之特徵性瘢痕形成(纖維化)及囊腫形成,於20世紀30年代首次確認。呼吸困難為最嚴重之症狀且由用抗生素及其他藥物治療之頻繁肺感染引起。其他症狀(包括竇感染、生長不良及不孕症)影響身體之其他部分。CF係由蛋白質囊腫性纖維化跨膜傳導調節子(CFTR)之基因突變引起。需要此蛋白質以調節汗液、消化液及黏液之組分。CFTR調節氯離子及鈉離子跨越上皮細胞膜(諸如位於肺中之肺泡上皮細胞)之運動。大多數不具有CF之人具有CFTR基因之兩個工作拷貝,且由於該病症之隱性性質,該兩個拷貝應為隱藏的以使CF發展。當兩個拷貝皆不能正常工作(由於突變)時形成CF且因此具有常染色體隱性遺傳性。在囊腫性纖維化及特發性肺纖維化之肥大細胞中進行研究,該等疾病具有外周肺纖維化作為顯著病理特徵(Andersson等人,(2011)「Activated MC(TC)mast cells infiltrate diseased lung areas in cystic fibrosis and idiopathic pulmonary
fibrosis」Respiratory Research 12(1),139)。儘管CF及IPF具有不同病因,但纖維變性病變之基本病理特徵包括過多膠原沈積。
在一些個體中,在無可鑒別原因之情況下形成慢性肺部炎症及纖維化。大部分此等個體具有稱為特發性肺纖維化(IPF)之病狀。IPF為一種病因不明之慢性進行性肺纖維化。潑尼松(prednisone)為IPF之常用治療,但IPF可用目標在於減少作為肺纖維化前奏之炎症的其他免疫抑制療法來治療。儘管潑尼松對改善肺功能具有適度可量測的作用,但對於其長期功效之證據缺乏以及關於其安全性之擔憂限制了其使用。實際上大部分免疫抑制藥物很少有治療作用且肺移植可能為必要的。遺憾的是,末期肺病患者中之移植成功率有限且患者之中位存活時間為診斷後四至六年。因而,需要新穎但有效之IPF治療。
關於特異性處理肺中纖維化之抑制或減緩之候選藥物(諸如IFN-γ及黴酚酸嗎啉乙酯(mycophenolate mofetil))的一些臨床試驗正在進行中。其他實施例包括:吡非尼酮,其作用機制並不明確,但似乎減少CTGF且已在臨床階段中顯示一些成果;經取代之聯苯羧酸,其充當溶血磷脂酸受體拮抗劑且在標準肺纖維化小鼠模型(博萊黴素誘發之肺纖維化)中顯示顯著的抗纖維變性活性。因而,據報導此化合物正處於IPF治療之臨床試驗中。用口服活性候選藥物抑制蛋白激酶或用口服活性抗氧化劑進行治療提供兩種對於肺纖維化之治療方法:多重激酶抑制劑(諸如尼達尼布(nintedanib))及JNK(激酶)抑制劑(諸如坦茲替布(tanzisertib))。此外,IPF候選藥物包括抗氧化劑N-乙醯基半胱胺酸。然而迄今為止,由於毒性及/或功效問題,蛋白激酶抑制劑及抗氧化劑之發展對於治療IPF一直是值得商榷的。在正常及病變細胞群體中普通存在蛋白激酶及相關受體,因此特定言之在迅速增殖之細胞群體中抑制作用會導致產生毒性。
另外,關於靶向用於治療IPF之不同促纖維變性蛋白(細胞介素(CTGF、TGF-β、MCP-1、IL-4及IL-13)、整合素(αvβ6)及酶(LOXL2酶)之單株抗體的臨床試驗正在進行中。然而,用於治療IPF之單株抗體(其應用於其他重組蛋白)的發展及使用產生許多相關問題,包括毒性(包括蛋白免疫原性)、製造難度(批次一致性、擴大規模、費用)及投予難度
(需要冷藏,而非口服活性)。
此外,雖然研究試驗正在進行,但無證據表明任何藥物治療可顯著有助於此病狀。肺移植為嚴重情況下唯一可用之治療選擇。遺憾的是,末期肺病患者中之移植成功率有限。因而,需要新穎但有效之IPF治療。因此,需要新穎但方便投予(口服活性)之有效的合成(容易製造)化合物。
肝纖維化
肝纖維化(liver fibrosis/hepatic fibrosis)為細胞外基質蛋白(包括膠原)之過度積聚以及後續瘢痕形成過程,其發生於大多數慢性肝病中。隨著時間推移,晚期肝纖維化導致肝硬化。肝硬化為慢性肝病之最終階段並且一般長期預後不良且不可逆。在晚期階段,唯一選擇為肝移植。肝硬化所伴隨之肝癌風險顯著增加且肝硬化可視為癌前病狀(肝細胞癌)。實際上,肝硬化及肝癌皆屬於全世界範圍內前十大死亡原因。因而,需要新穎但有效的對肝纖維化及後續肝硬化之治療。遺憾的是,可用治療選擇很少且最通常治療由處理肝硬化之病因及/或症狀組成。尚無治療可治癒肝纖維化後續之瘢痕形成及肝硬化。肝移植為晚期纖維化患者唯一可用之治療。因此,需要侵入性較小之替代性方法來治癒肝纖維化、治療肝纖維化、減緩肝纖維化之進展或預防肝纖維化。
腹部流體(腹水)積聚為與肝硬化相關之常見問題。治療選擇包括低鈉飲食、利尿劑以及藉由插入針於腹腔中(腹腔穿刺)來移除流體。肝硬化由酒精濫用、病毒性肝炎(B、C及D)、與肥胖症相關之非酒精性脂肪肝病(NAFLD)、糖尿病、蛋白質營養不良、冠狀動脈疾病、皮質類固醇、自體免疫肝炎、遺傳性疾病(囊腫性纖維化、α-1-抗胰蛋白酶缺乏症等)、原發性膽汁性肝硬化、藥物反應及暴露於毒素引起。
關於特異性處理肝纖維化之抑制或減緩之候選藥物的有限數目之臨床試驗正在進行中。然而,此等試驗針對特定肝病,諸如NASH(非酒精性脂肪肝炎)。NASH係指脂肪肝(NAFLD)與炎症之組合且發生於飲酒很少或不飲酒之個體中。半胱胺為有效的肝抗氧化劑麩胱甘肽之前
驅體且鹹信麩胱甘肽之活體內產生增加提供NASH相關肝病之改善。因而,半胱胺正在NASH兒童患者中進行臨床試驗評估。其他抗氧化劑諸如維生素E及硒正在進行評估,但其用於治療NASH之效用未知。此外處於NASH治療評估中的是甚至在不具有糖尿病之患者中使用抗糖尿病藥物。此方法處理了大多數NASH患者具有胰島素抗性之事實。再次,需要新穎但方便投予(口服活性)之用於治療肝纖維化、後續瘢痕形成及肝硬化的有效化合物。
皮膚纖維化
皮膚纖維化(skin fibrosis/dermal fibrosis)為皮膚之過度瘢痕形成,且為病理性傷口癒合反應之結果。存在廣泛多種纖維變性皮膚疾病:硬皮病、腎源性纖維化皮膚病、混合性結締組織疾病、硬化性黏液水腫、硬腫病及嗜酸性筋膜炎。暴露於化學物質或物理因素(機械創傷、燒傷創面)亦為纖維變性皮膚疾病之潛在原因。皮膚纖維化可由免疫、自體免疫及炎症機制驅動。膠原產生與由纖維母細胞降解的平衡在皮膚中之纖維變性過程之病理生理學中起關鍵作用。某些細胞介素促進傷口癒合及纖維化,諸如轉化生長因子-β(TGF-β)及介白素-4(IL-4),而其他細胞介素抗纖維變性,諸如幹擾素-γ(IFN-γ)及腫瘤壞死因子-α(TNF-α)。正常皮膚之纖維母細胞處於靜止狀態。其合成受控量之結締組織蛋白且具有低增殖活性。在皮膚損傷後,此等細胞變得活化,亦即其增殖、表現α-平滑肌肌動蛋白(α-SMA)且合成大量結締組織蛋白。該等活化細胞通常稱為肌纖維母細胞。
在皮膚纖維化期間,自美容觀點來看,作為傷口癒合過程之一部分且伴隨著纖維化之瘢痕形成為特別不合需要的,尤其當瘢痕形成於面部及/或身體之其他暴露部分上時。硬皮病(scleroderma)係指皮膚纖維化;sclera表示硬且derma表示皮膚。然而,皮膚纖維化可能具有重要的健康問題,尤其當其為全身性硬皮病之一部分時。全身性硬皮病係指具有自體免疫病因之結締組織疾病。局限皮膚型硬皮病受限於面部上及足部上之皮膚,而彌漫皮膚型硬皮病覆蓋更多皮膚且可發展至內臟器官。
用於治療皮膚纖維化之最流行的方法為使用免疫抑制療法。基本原理在於,自體免疫病因造成疾病之炎症態樣以及後續組織損傷及纖維化。所研究之藥物包括甲胺喋呤、黴酚酸嗎啉乙酯、環磷醯胺及環孢靈(cyclosporine)。儘管已觀測到免疫抑制療法之一些改進,但關於藥物安全性之擔憂以及確定之臨床資料及可證實之功效的缺乏仍然存在。
需要開發用於治療皮膚纖維化、纖維變性皮膚疾病及皮膚之病理性瘢痕形成的有效醫藥製劑。
心臟纖維化
心臟纖維化(心臟疾病之標誌)被認為促進心臟性猝死、心室性心動過速、左心室(LV)功能障礙及心臟衰竭。心臟纖維化之特徵在於心肌細胞死亡後發生之原纖化膠原的不相稱積聚、炎症、工作負荷增強、肥厚,以及受多種激素、細胞介素及生長因子的刺激。
心臟纖維化亦可指心臟瓣膜由於心臟纖維母細胞之不當增殖而引起的異常增厚,但更通常指心肌中纖維母細胞之增殖。纖維細胞通常分泌膠原,且用於對心臟提供結構支撐。當過度活化時,此過程造成瓣膜增厚及纖維化,其中白色組織主要聚集於三尖瓣上,但亦存在於肺動脈瓣上。增厚及柔性損失最終可導致瓣膜功能不全及右側心臟衰竭。
用於心臟瓣膜纖維化或其他部位纖維化之最明顯治療由停用刺激性藥物或產生血清素組成。在一些患者中有必要為嚴重狹窄(阻塞血流)進行手術三尖瓣置換。此外,已發現紅葡萄酒中存在之化合物白藜蘆醇(resveratrol)可減緩心臟纖維化之發展。[Olson等人,(2005)「Inhibition of cardiac fibroblast proliferation and myofibroblast differentiation by resveratrol」.American journal of physiology. Heart and circulatory physiology 288(3):H1131-8;Aubin等人,(2008)「Female rats fed a high-fat diet were associated with vascular dysfunction and cardiac fibrosis in the absence of overt obesity and hyperlipidemia:Therapeutic potential of resveratrol」.The Journal of Pharmacology and Experimental Therapeutics 325(3):961-8。]正在於動物模型中測試抵抗心臟纖維化之更先進方法如微RNA抑制(例如miR-21)。
市面上不存在用於預防或治療心臟纖維化之藥物且需要開
發有效之醫藥製劑。
依據本發明之一實施例,係特地提出一種用於在有需要之個體中預防纖維變性疾病及/或減緩纖維變性疾病之進展及/或治療纖維變性疾病的方法,其中該纖維變性疾病為肺纖維化、肝纖維化、皮膚纖維化或心臟纖維化,該方法包括投予治療有效量的由下式表示之化合物:
1)(CH2)mC(O)OH,其中m為1或2,
2)CH(CH3)C(O)OH,
3)C(CH3)2C(O)OH,
4)CH(F)-C(O)OH,
5)CF2-C(O)OH,或
6)C(O)-C(O)OH。
圖1展示相比於用媒劑(水)(博萊黴素)經口處理,在用劑量為100mg/kg及200mg/kg之化合物I經口處理之後,在博萊黴素誘發之肺纖維化小鼠模型中的體重減輕恢復。
圖2展示在用劑量為100mg/kg及200mg/kg之化合物I經
口處理或用媒劑(水)(博萊黴素)經口處理之後,使用HEP(Hemalun與曙紅(Eosin)/玫瑰紅(Ploxine))及Masson三色染色對來自博萊黴素誘發之肺纖維化小鼠模型之肺組織學樣本進行評估,顯示病變顯著減少。
圖3展示在用劑量為100mg/kg及200mg/kg之化合物I經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織的顯微照片。
圖4展示在用劑量為100mg/kg及200mg/kg之化合物I經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織的CTGF含量。使用大鼠CTGF TaqMan®基因表現檢定之即時PCR相對於大鼠Gapdh內源性對照物進行校正。
圖5展示在用劑量為100mg/kg及200mg/kg之化合物I經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織的IL-23p19含量。使用大鼠IL-23p19 TaqMan®基因表現檢定之即時PCR相對於大鼠Gapdh內源性對照物進行校正。
圖6展示在用劑量為100mg/kg及200mg/kg之化合物I經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織的膠原1含量。使用大鼠膠原1 TaqMan®基因表現檢定之即時PCR相對於大鼠Gapdh內源性對照物進行校正。
圖7展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合或媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之受博萊黴素影響之肺的百分比。
圖8展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之受博萊黴素影響之肺以及正常小鼠(無博萊黴素)之肺組織(對照物)的組織學病變評分。
圖9展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑
(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之受博萊黴素影響之肺以及正常小鼠(無博萊黴素)之肺組織(假處理組)的病變評分,該評分係藉由白血球浸潤百分比(炎性區域)乘以白血球浸潤物中存在之膠原百分比測定且藉由使用Masson三色染色之組織形態測量術定量。
圖10展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自用HEP染色之博萊黴素誘發之肺纖維化小鼠模型之肺組織的顯微照片。
圖11展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺以及正常小鼠(無博萊黴素)之肺組織(對照物)的Ashcroft評分所確定的肺纖維化目測等級。
圖12展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織以及正常小鼠(無博萊黴素)之肺組織(對照物)的TGF-β mRNA含量。
圖13展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織以及正常小鼠(無博萊黴素)之肺組織(對照物)的CTGF mRNA含量。
圖14展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織以及正常小鼠(無博萊黴素)之肺組織(對照物)的IL-23p19 mRNA含量。
圖15展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織以及正常小鼠(無博萊黴素)之肺組織(對照物)的IL-6 mRNA含量。
圖16展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織以及正常小鼠(無博萊黴素)之肺組織(對照物)的膠原1 mRNA含量。
圖17展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織以及正常小鼠(無博萊黴素)之肺組織(對照物)的纖維結合蛋白(FN-1)mRNA含量。
圖18展示在用化合物I(200mg/kg)、吡非尼酮(400mg/kg)、化合物I(200mg/kg)與吡非尼酮(400mg/kg)之組合經口處理或用媒劑(水)(博萊黴素)經口處理之後,來自博萊黴素誘發之肺纖維化小鼠模型之肺組織以及正常小鼠(無博萊黴素)之肺組織(對照物)的膠原3 mRNA含量。
圖19展示在每天經口投予化合物I或經口投予媒劑(水)(CCl4)之後,來自CCl4誘發之肝纖維化小鼠模型之肝以及來自正常小鼠(無CCl4)之肝(對照物)中的羥脯胺酸含量。
圖20展示在每天經口投予化合物I或經口投予媒劑(水)(CCl4)之後,來自CCl4誘發之肝纖維化小鼠模型之肝中的膠原含量。
圖21展示在每天經口投予化合物I(200mg/kg)或經口投予媒劑(水)(CCl4)之後,來自CCl4誘發之肝纖維化小鼠模型之肝以及來自正常小鼠(無CCl4)之肝(對照物)的顯微照片。
圖22展示在每天經口投予劑量為100mg/kg及200mg/kg
之化合物I及化合物V或經口投予媒劑(水)(CCl4)之後,來自CCl4誘發之肝纖維化小鼠模型之肝中藉由組織形態量測術(Masson三色染色)測定的全部肝區中之膠原含量百分比。
圖23展示用單獨化合物I(0.5mM)、單獨TGF-β或兩者之組合或兩者皆不存在情況下(未經處理)培養之正常人類皮膚纖維母細胞(NHDF)中的CTGF mRNA含量。使用人類CTGF TaqMan®基因表現檢定之即時PCR相對於人類GAPDH內源性對照物進行校正;參考為經TGF-β處理之細胞(RQ=1)。
圖24展示用單獨化合物I(0.5mM)、單獨TGF-β或兩者之組合或兩者皆不存在情況下(未經處理)培養之正常人類皮膚纖維母細胞(NHDF)中的膠原1 mRNA含量。使用人類膠原1 TaqMan®基因表現檢定之即時PCR相對於人類GAPDH內源性對照物進行校正;參考為經TGF-β處理之細胞(RQ=1)。
圖25展示用單獨化合物I(0.5mM)、單獨TGF-β或兩者之組合或兩者皆不存在情況下(未經處理)培養之正常人類皮膚纖維母細胞(NHDF)中的α-SMA mRNA含量。使用人類α-SMA TaqMan®基因表現檢定之即時PCR相對於人類GAPDH內源性對照物進行校正;參考為經TGF-β處理之細胞(RQ=1)。
圖26展示在化合物I(0.5mM)存在及不存在下培養之正常人類皮膚纖維母細胞(NHDF)的刮痕檢定(遷移及入侵檢定),顯示經處理細胞在刮痕中之遷移及入侵減少。
圖27展示相比於未植入導管之5/6-Nx大鼠(NX)且相比於非腎切除大鼠(假處理組),在5/6-Nx大鼠中使用導管(具有導管之NX)誘導心臟病變程度增加。
圖28展示相比於未經處理之5/6-Nx大鼠(NX),在靜脈內(iv)投予化合物I或經口(po)投予化合物I之後,來自5/6腎切除-經插入導管(5/6-Nx)大鼠之心臟中藉由組織學評估(HPE及Masson三色染色)所測定的病變程度。
圖29展示相比於未經處理之5/6-Nx大鼠(NX),在靜脈內
(iv)投予化合物I或經口(po)投予化合物I之後,來自5/6腎切除-經插入導管(5/6-Nx)大鼠之心臟中的炎症程度。
圖30展示相比於未經處理之5/6-Nx大鼠(NX),在靜脈內(iv)投予化合物I或經口(po)投予化合物I之後,來自5/6腎切除-經插入導管(5/6-Nx)大鼠之心臟中的壞死程度。
圖31展示相比於未經處理之5/6-Nx大鼠(NX)及非腎切除大鼠(假處理組),在靜脈內(iv)投予化合物I或經口(po)投予化合物I之後,來自5/6腎切除-經插入導管(5/6-Nx)大鼠之心臟中的羥脯胺酸(膠原)含量。
圖32展示藉由經口投予化合物I處理之5/6腎切除-經插入導管(5/6-Nx)大鼠及未經處理之5/6-Nx大鼠(NX)之心臟的40倍放大視圖顯微照片。
圖33展示藉由經口投予化合物I處理之5/6腎切除-經插入導管(5/6-Nx)大鼠及未經處理之5/6-Nx大鼠(NX)之心臟的100倍放大視圖顯微照片。
圖34展示藉由靜脈內投予化合物I處理之5/6腎切除-經插入導管(5/6-Nx)大鼠及未經處理之5/6-Nx大鼠(NX)之心臟的40倍放大視圖顯微照片。
令人驚訝的是,本發明人已確定本發明化合物於肺、肝臟、皮膚及心臟中顯示抗纖維變性活性。已知本發明化合物具有良好的安全性概況;本發明人推斷,本發明化合物為用於預防/治療肺纖維化、肝纖維化、皮膚纖維化及心臟纖維化之優良藥物候選物。心臟纖維化(Cardiac fibrosis)與心臟纖維化(heart fibrosis)在本文可互換使用且意欲指示相同物。
更特定言之,本發明關於一種用於在有需要之個體中預防纖維變性疾病及/或減緩纖維變性疾病之進展及/或治療纖維變性疾病的方
法。該纖維變性疾病為肺纖維化、肝纖維化、皮膚纖維化或心臟纖維化。該方法包括投予治療有效量的由下式表示之化合物:
或其醫藥學上可接受之鹽,其中
A為C5烷基、C6烷基、C5烯基、C6烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為3或4;或較佳為C5烷基、C5烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為3;或較佳為C6烷基、C6烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為4;
R1為H、OH或F;或較佳為H或OH;
R2為H、OH、F或CH2-OH;或較佳為H、OH或F;或較佳為H或OH;
R3為H、OH、F或CH2Ph;或較佳為H、OH或F;或較佳為H或OH;
R4為H、OH或F;或較佳為H或OH;
Q為
1)(CH2)mC(O)OH,其中m為1或2,
2)CH(CH3)C(O)OH,
3)C(CH3)2C(O)OH,
4)CH(F)-C(O)OH,
5)CF2-C(O)OH,或
6)C(O)-C(O)OH。
在一較佳實施方案中,化合物之醫藥學上可接受之鹽為鈉鹽、鉀鹽、鋰鹽、銨鹽、鈣鹽、鎂鹽、錳鹽、鋅鹽、鐵鹽或銅鹽。較佳的化合物之醫藥學上可接受之鹽為鈉鹽。
根據本發明之一較佳實施方案,該化合物為下列化合物之一:
在一實施方案中,纖維變性疾病為肺纖維化。在此實施方案中,治療有效量較佳為約1mg/kg至約50mg/kg,且較佳為約1mg/kg至約20mg/kg。化合物較佳經口投予。個體較佳為人類。根據本發明之一較佳實施方案,肺纖維化為特發性肺纖維化、肉狀瘤病、囊腫性纖維化、家族性肺纖維化、矽肺病、石綿沈著病、煤礦工人塵肺病、碳塵肺病、過敏性肺
炎、由吸入無機粉塵引起之肺纖維化、由感染物引起之肺纖維化、由吸入有毒氣體、氣溶膠、化學粉塵、煙霧或蒸氣引起之肺纖維化、藥物誘發之間質性肺病或肺性高血壓。
在一實施方案中,纖維變性疾病為肝纖維化。在此實施方案中,治療有效量較佳為約1mg/kg至約50mg/kg。化合物較佳經口投予。個體較佳為人類。根據本發明之一較佳實施方案,肝纖維化由慢性肝病、B型肝炎病毒感染、C型肝炎病毒感染、D型肝炎病毒感染、血吸蟲病、酒精性肝病或非酒精性脂肪肝炎、肥胖症、糖尿病、蛋白質營養不良、冠狀動脈疾病、自體免疫肝炎、囊腫性纖維化、α-1-抗胰蛋白酶缺乏症、原發性膽汁性肝硬化、藥物反應及暴露於毒素引起。
在一實施方案中,纖維變性疾病為皮膚纖維化。在此實施方案中,化合物較佳經局部或經口投予。當經局部投予時,本發明化合物之治療有效量較佳為約0.01%至約10%(w/w)。個體較佳為人類。當經口投予時,本發明化合物之治療有效量較佳為約1mg/kg至約50mg/kg且個體為人類。根據本發明之一較佳實施方案,皮膚纖維化為瘢痕形成、增生性瘢痕形成、瘢痕瘤、皮膚纖維變性病症、傷口癒合、傷口延遲癒合、牛皮癬或硬皮病。該瘢痕形成可能源自燒傷、創傷、手術損傷、輻射或潰瘍。該潰瘍可為糖尿病性足潰瘍、靜脈性腿潰瘍或壓力性潰瘍。
在一實施方案中,纖維變性疾病為心臟纖維化。在此實施方案中,治療有效量較佳為約1mg/kg至約50mg/kg,且較佳為約1mg/kg至約20mg/kg。該化合物較佳經口投予。該個體較佳為人類。
除先前劑量實施方案之外,對於所有上述纖維變性疾病,當本發明化合物經口投予人類時,化合物之治療有效量較佳對應於約0.01%至約10%(w/w)、或約0.1%至10%(w/w)、或約1.0%至約10%(w/w)、約0.1%至約5%(w/w)、或約1.0%至約5%(w/w)。在所有上述纖維變性疾病中,當本發明化合物經口投予人類時,化合物之治療有效量較佳對應於約1mg/kg至約50mg/kg、或約1mg/kg至25mg/kg、或約1mg/kg至約10mg/kg、約5mg/kg至約25mg/kg、或約10mg/kg至約20mg/kg。
根據一較佳實施方案,本發明亦關於一種用於拮抗哺乳動物
之器官(諸如肺、肝臟、皮膚或心臟)中之膠原分泌或膠原沈積的方法,其包括向有需要之該哺乳動物投予治療有效量之本發明化合物,其中該器官為肺、肝臟、皮膚或心臟。有需要之哺乳動物為在諸如肺、肝臟、皮膚或心臟之器官中經受過多膠原分泌或膠原沈積的哺乳動物。通常,器官中之過多膠原分泌或膠原沈積由損傷或傷害引起。該等損傷及傷害具器官特異性且于本文詳細描述於先前技術部分及整個說明書中。上文詳細描述之治療有效量亦適用於拮抗器官中之膠原分泌或膠原沈積之本方法。本文所述之投予途徑亦適用於本方法。該化合物較佳經足夠時段投予以完全或部分拮抗器官中之膠原沈積水準。本文所用之術語「拮抗」欲意謂「降低」或「減少」。足夠時段可為在一周內、或1周至1個月、或1至2個月、或2個月以上。對於慢性病狀,本發明化合物宜終生投予。
本發明亦關於一種用於減少細胞中之膠原產生之方法,其包括使該等細胞與治療有效量之本發明化合物接觸。該膠原較佳為膠原1。該膠原產生較佳為膠原mRNA表現或膠原蛋白產生。根據一較佳實施方案,細胞處於培養中,為器官之一部分或為完全為活動物之一部分之器官的一部分,其中該動物包括但不限於小鼠、大鼠或人類。在細胞為完全為活動物之一部分之器官的一部分的情況下,使細胞與治療有效量之本發明化合物接觸的步驟等效于向動物投予化合物。在細胞為完全為活動物之一部分之器官的一部分且活動物為人類的情況下,化合物之治療有效量對應於較佳約0.01%至約10%(w/w)、或約0.1%至10%(w/w)、或約1.0%至約10%(w/w)、約0.1%至約5%(w/w)、或約1.0%至約5%(w/w)之局部投予量,或對應於較佳約1mg/kg至約50mg/kg、或約1mg/kg至25mg/kg、或約1mg/kg至約10mg/kg、約5mg/kg至約25mg/kg、或約10mg/kg至約20mg/kg之經口投予量。在培養細胞之情況下,化合物之治療有效量對應於0.01mM至0.5mM,且較佳為約0.2mM。
在另一較佳實施方案中,本發明化合物與治療有效量之第二化合物組合投予,其中該第二化合物較佳為已知可有效預防或治療或潛在預防或治療肺纖維化、肝纖維化或皮膚纖維化的治療劑。在另一較佳實施方案中,該化合物與治療有效量的第二化合物組合投予,該第二化合物為
免疫抑制藥物、消炎藥物、細胞介素、單株抗體、多重受體酪胺酸激酶抑制劑、抗氧化劑、酶抑制劑、整合素抑制劑、脂質受體調節劑或噻唑啉二酮。
在纖維變性疾病為肺纖維化之一較佳實施方案中,本發明化合物與治療有效量之吡非尼酮組合投予。在此情況下,較佳化合物為化合物I。在受肺纖維化影響之個體為人類的情況下,當經口投予時,化合物I之治療有效量為約1mg/kg至約50mg/kg、或約1mg/kg至25mg/kg、或約1mg/kg至約10mg/kg、約5mg/kg至約25mg/kg、或約10mg/kg至約20mg/kg,且吡非尼酮為約10mg/kg至約40mg/kg、或約1.0公克/天至約2.5公克/天。本發明化合物與第二治療劑之組合可於單一製劑中或於獨立製劑中投予。
本發明亦關於一種用於在有需要的個體中預防纖維變性疾病及/或減緩纖維變性疾病之進展及/或治療纖維變性疾病的套組。該套組包含由下式表示之化合物:
或其醫藥學上可接受之鹽,其中
A為C5烷基、C6烷基、C5烯基、C6烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為3或4;或較佳為C5烷基、C5烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為3;或較佳為C6烷基、C6烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為4;
R1為H、OH或F;或較佳為H或OH;
R2為H、OH、F或CH2-OH;或較佳為H、OH或F;或較佳為H或OH;
R3為H、OH、F或CH2Ph;或較佳為H、OH或F;或較佳為H或OH;
R4為H、OH或F;或較佳為H或OH;
Q為
1)(CH2)mC(O)OH,其中m為1或2,
2)CH(CH3)C(O)OH,
3)C(CH3)2C(O)OH,
4)CH(F)-C(O)OH,
5)CF2-C(O)OH,或
6)C(O)-C(O)OH;
以及關於向罹患該纖維變性疾病之個體投予治療有效量之該化合物的說明書,其中該纖維變性疾病為肺纖維化、肝纖維化、心臟纖維化或皮膚纖維化。
當纖維變性疾病為肺纖維化、心臟纖維化或肝纖維化時,該套組較佳進一步包含關於向人類個體每天經口投予約1mg/kg至約50mg/kg化合物的說明書。該套組亦可包含關於投予任何上文揭示之治療有效量之經口投予化合物的說明書。
當纖維變性疾病為皮膚纖維化時,該套組較佳進一步包含關於向人類個體每天經局部投予約0.01%至約10%(w/w)之化合物的說明書;或關於向人類個體每天經口投予約1mg/kg至約50mg/kg化合物的說明書。該套組亦可包含關於投予任何上文揭示之治療有效量之經局部投予化合物的說明書。
本發明亦關於由下式表示之新穎化合物:
或其醫藥學上可接受之鹽,其中
A為C5烷基、C6烷基、C5烯基、C6烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為3或4;
R1為H、OH或F;
R2為H、OH、F或CH2-OH;
R3為CH2Ph;
R4為H、OH或F;
Q為
1)(CH2)mC(O)OH,其中m為1或2,
2)CH(CH3)C(O)OH,
3)C(CH3)2C(O)OH,
4)CH(F)-C(O)OH,
5)CF2-C(O)OH,或
6)C(O)-C(O)OH。
此化合物之較佳實施方案為具有以下結構之化合物XX:
如本文所用,術語「烷基」意欲包括具有五個或六個碳原子之支鏈及直鏈飽和脂族烴基。上文定義之烷基的實例包括但不限於正戊基、正己基、異戊基、異己基、第三戊基及第三己基。類似地,如本文所用,術語「烯基」意欲包括具有五個或六個碳原子且其中至少兩個碳原子由雙鍵彼此鍵結且具有E或Z區域化學及其組合的不飽和直鏈或支鏈烴基。上文定義之烯基的實例包括但不限於1-戊烯基、2-戊烯基、1-己烯基及2-己烯基。
本發明化合物或其醫藥學上可接受之鹽可含有一或多個不對稱中心、手性軸及手性平面,且因此可產生對映異構體、非對映異構體及其他立體異構形式,隨後可根據絕對立體化學諸如(R)-或(S)-進行定義。因此本發明意欲包括所有此等可能的異構體,以及其外消旋及光學純形式。光學活性(+)及(-)、(R)-及(S)-或(D)-及(L);異構體可使用手性合成子或手性試劑製備或使用習知技術諸如逆相HPLC離析。外消旋混合物可經製備且隨後分離為個別光學異構體或此等光學異構體可藉由手性合成來製備。對映異構體可藉由熟習此項技術者已知之方法離析,例如,藉由形成非對映異構鹽,其隨後可藉由結晶、氣相-液相或液相層析分離,或使一種對映異構體與對映異構體特異性試劑選擇性反應。
如本文所用,術語「醫藥學上可接受之鹽」欲意謂保持自由酸之生物效能及特性且在生物學上或在其他方面非不合需要之彼等鹽。此等鹽衍生自無機鹼或有機鹼與有機酸之加成。由無機鹼製備之鹽包括但不限於鈉鹽、鉀鹽、鋰鹽、銨鹽、鈣鹽、鎂鹽、錳鹽、鋅鹽、鐵鹽、銅鹽及其類似物。由有機鹼製備之鹽包括但不限於以下各物之鹽:一級、二級及三級胺、經取代之胺(包括天然存在之經取代之胺)、環胺及鹼性胺基酸(離胺酸、精胺酸及組胺酸)。醫藥學上可接受之鹽的實例亦描述於例如Berge等人,「Pharmaceutical Salts」,J.Pharm.Sci.66,1-19(1977)中。本發明化合物之較佳鹽為鈉鹽、鉀鹽、鋰鹽、銨鹽、鈣鹽及鎂鹽;且更佳為鈉鹽。醫藥學上可接受之鹽可藉由習知化學方法由含有酸部分之母體化合物合成。一般而言,此等鹽係藉由使此等化合物之自由酸形式與化學計算量之適當鹼于水中或於有機溶劑中或於水性/有機溶劑混合物中反應來製備。鹽可在
化合物之最終分離或純化期間就地製備或藉由分別使自由酸形式之經純化本發明化合物與所需相應鹼反應且分離產物鹽來製備。
如上文所指示及下文所例示,本發明化合物具有有益之醫藥特性並且可具有用於預防及/或治療個體中之各種疾病及病狀的醫藥應用。本發明人所預期之藥學及醫藥應用包括但不限於處理肺纖維化、肝纖維化、心臟纖維化及皮膚纖維化之彼等應用。
術語「個體」包括可能發生肺纖維化或易於患上此病狀之活有機體。術語「個體」包括動物,諸如哺乳動物或鳥類。個體較佳為哺乳動物。個體更佳為人類。個體甚至更佳為需要治療之人類患者。
如本文所用,「預防」欲指至少降低獲得疾病或病症之風險(或易感性)的可能性(亦即,在可能患上或易患上疾病但尚未經歷或顯示該疾病之症狀的患者中造成該疾病之至少一種臨床症狀未出現)。用於鑒別此等患者之生物及生理參數提供于本文中且亦為醫師所熟知。
術語個體之「治療」包括向個體施用或投予本發明化合物(或向來自個體之細胞或組織施用或投予本發明化合物),目的在於延遲、減緩、穩定化、治療、治癒、緩解、減輕、改變、醫治、減少惡化、改善、改進或影響疾病或病狀、疾病或病狀之症狀、或疾病或病狀之風險(或易感性)。術語「治療」係指損傷、病變或病狀之治療或改善成功的任何指示,包括任何客觀或主觀參數,諸如消除;緩解;惡化速率減小;疾病嚴重程度減小;穩定化、減輕症狀或使個體更耐受損傷、病變或病狀;減緩惡化或衰退之速率;使惡化終點之衰弱程度較小;或改善個體之身體或精神健康狀況。
本發明係關於用於預防及/或治療有需要之個體之肺纖維化、肝纖維化、心臟纖維化或皮膚纖維化的方法、化合物、組成物及套組。
術語「肺纖維化」意謂肺中形成或產生過多纖維結締組織(纖維化),從而導致產生瘢痕化(纖維變性)組織。更確切地說,肺纖維化為造成肺泡及肺間質組織腫脹及瘢痕形成之慢性疾病。瘢痕組織置換健康組織且造成炎症。此慢性炎症又為纖維化之前奏。此種對肺組織之損傷造成肺變硬,隨後使呼吸愈來愈困難。
肺纖維化為可由許多不同原因引起之複雜疾病,該等原因包括因吸入小粒子(石棉、磨細石料、金屬粉塵、香煙煙霧中存在之粒子、二氧化矽粉塵等)誘發之肺部微觀損傷。或者,肺纖維化可作為其他疾病(自體免疫疾病、病毒性或細菌性感染等)之副作用而出現。某些藥物,諸如細胞毒性劑(例如博萊黴素、白消安及甲胺喋呤)、抗生素(例如呋喃妥因、柳氮磺胺吡啶)、抗心律失常藥(例如胺碘達隆(amiodarone)、妥卡胺(tocainide))、消炎藥物(例如金、青黴胺)、違禁藥物(例如快克可卡因、海洛因),亦可造成肺纖維化。然而,當在無已知原因下出現肺纖維化時,將其稱為「特發性」或特發性肺纖維化(IPF)。
肺纖維變性病症被認為是起始於肺實質之急性損傷,其導致慢性間質性炎症,隨後纖維母細胞活化及增殖,且最終發展為肺纖維化及組織破壞之常見終點。當前研究表明,炎症在IPF中不甚重要,IPF似乎主要為回應一些未知觸發之纖維母細胞活化及增殖病症。廣義而言,纖維變性肺部疾病之表現可以歸納如下:其可為慢性、隱伏性及緩慢進行性的;其可為亞急性的,具有消散性、緩解性、復發性或進行性過程;以及其可為急性的,具有爆發性、進行性、緩解性或消散性過程。具有慢性、隱伏性及緩慢進行性過程之病症為臨床上類似於IPF且通常有共同病理學者(亦即UIP)。許多結締組織疾病(例如類風濕性關節炎;CREST症候群(皮膚鈣沈著症、雷諾氏症候群(Raynaud's syndrome)、食管運動障礙、指硬皮病及毛細管擴張症);症候群/進行性全身性硬皮病;全身性紅斑狼瘡;混合性結締組織疾病;塵肺病(例如石綿沈著病、矽肺病);慢性過敏性肺炎;及藥物相關之肺纖維化(例如由於博萊黴素))一般屬於此類別。與職業暴露相關之臨床上明顯之肺部疾病(例如塵肺病)的發展一般在暴露後很多年才出現。輻射性纖維化通常在輻射曝露後數月至數年才出現。在使用肺毒性藥物與產生纖維變性疾病之間可能出現數月或數年之滯後時間。該作用可為劑量依賴性(例如博萊黴素),但在其他情況下,關係不甚明顯。結締組織疾病之肺部表現可能在關節疾病發作之前、同時或很多年後才出現。肺部肉狀瘤病儘管有時急性或亞急性發作,但在一些情況下可能隨時間隱伏存在。具有可變過程之亞急性表現以隱源性機化肺炎(COP)為代表。
COP通常在流感樣疾病發作後數周或數月才出現。該過程為可變的且可自發緩解或進展。該病症被認為對類固醇療法極具反應性,但當類固醇類撤除或逐漸減少時其可再次出現。在一些情況下,COP可進展為末期纖維變性肺部疾病。具有急性發作之病症以急性間質性肺炎(AIP)為代表,其為重度肺損傷之特發形式。組織病理學為具有彌漫性肺泡損傷之成人呼吸窘迫症候群之組織病理學。患者不具有早先肺病史或存在潛在間質性疾病之加速期的一部分。大多數患者迅速進展為呼吸衰竭。一些患者可用類固醇類或其他免疫抑制療法進行改善。
術語「肝纖維化」意謂肝臟中形成或產生過多纖維結締組織(纖維化),從而導致產生瘢痕化(纖維變性)組織。瘢痕化組織藉由纖維化過程置換健康組織且導致後續肝硬化。
術語「皮膚纖維化」意謂上皮細胞或纖維結締組織之過度增殖(纖維化),從而導致產生瘢痕化(纖維變性)組織。瘢痕化組織藉由纖維化過程置換健康組織且可為全身性硬皮病之前奏。皮膚纖維化意欲涵蓋任何皮膚組織及上皮細胞之纖維化,包括但不限於血管及靜脈、器官或腺體之內腔諸如下頜下、膽囊、甲狀腺毛囊、汗腺管、卵巢、腎臟之導管;齒齦、舌、齶、鼻、喉、食道、胃、腸、直腸、肛門及陰道之上皮細胞;真皮、瘢痕、皮膚及頭皮。本發明化合物可有效促進傷口癒合且具有一或多種下列活性:
- 改善膠原組織化及/或減少該傷口中之傷口多孔性;
- 減少該傷口中由纖維母細胞及上皮細胞產生之膠原過度產生;
- 減少該傷口中之上皮間質轉化;
- 減少該傷口中之纖維母細胞遷移及活化;
- 減少及/或抑制該傷口中之皮膚增厚;
- 減少及/或抑制炎性細胞向該傷口之募集。
術語「心臟纖維化」意謂心臟瓣膜由於心臟纖維母細胞之不當增殖而引起的異常增厚,但更通常指心肌中纖維母細胞之增殖。纖維細
胞通常分泌膠原,且用於對心臟提供結構支撐。當過度活化時,此過程造成瓣膜增厚及纖維化,其中白色組織主要聚集於三尖瓣上,但亦存在於肺動脈瓣上。增厚及柔性損失最終可導致瓣膜功能不全及右側心臟衰竭。
一般而言,預防性及治療性用途包括向有需要之個體、較佳人類患者投予如本文所述之化合物。
根據本發明之化合物可與治療有效量之第二化合物組合投予,該第二化合物可包括於相同的醫藥組成物中或第二醫藥組成物中。該第二化合物宜為免疫抑制藥物,包括但不限於環孢靈、硫唑嘌呤、環磷醯胺或黴酚酸嗎啉乙酯;消炎藥物,包括但不限於皮質類固醇(例如潑尼松);細胞介素,包括但不限於幹擾素-α、幹擾素-γ、介白素12;單株抗體,包括但不限於CTGF、TGF-β、MCP-1、IL-4及IL-13;多重受體酪胺酸激酶抑制劑,包括但不限於尼達尼布及JNK(激酶)抑制劑坦茲替布(CC-930);抗氧化劑,諸如但不限於N-乙醯基半胱胺酸、吡非尼酮(pirfenidone)、維生素E、S-腺苷甲硫胺酸或青黴胺;酶抑制劑,包括但不限於離胺醯氧化酶樣2(LOXL2酶);整合素抑制劑,例如但不限於αvβ6;脂質受體調節劑,包括但不限於溶血磷脂酸受體拮抗劑;或噻唑啉二酮或吡非尼酮。
本發明之一相關態樣關於包含一或多種本文所述之本發明化合物的醫藥組成物及套組。如上文所指示,本發明化合物可用於預防及/或治療肺纖維化、肝纖維化、心臟纖維化及皮膚纖維化。
本發明之一相關態樣關於與肺纖維化、肝纖維化、心臟纖維化及皮膚纖維化有關之化合物的預防性及治療性用途。肺纖維化可導致若干嚴重併發症。因為纖維變性之肺部的氧攝入能力受損,所以可能產生低血氧含量(低血氧症)。氧缺乏可能影響整個身體。肺纖維化之另一併發症為肺性高血壓(肺動脈高血壓)。肺部瘢痕組織可使得血液更難以流過。壓力增加使得心臟負荷更大且導致心臟衰弱並擴張,使其泵送效率降低並產生心臟衰竭。當人們產生腹部流體積聚、腿部腫脹或頸靜脈脈動顯著時,疑似此病症。
肝纖維化可導致嚴重的肝臟機能不良且可導致肝臟完全失去功能。
在因手術或事故造成之皮膚損傷後,皮膚纖維化可導致雜亂印記、永久傷痕及瘢痕,造成嚴重的美觀問題及皮膚變硬。
心臟纖維化可導致嚴重的心臟機能不良及死亡。
如本文所用,術語「治療有效量」意謂當投予個體用於治療或預防特定病症、疾病或病狀時,足以實現該病症、疾病或病狀之此種治療或預防的化合物量。劑量及治療有效量可例如根據多種因素而改變,該等因素包括所用特定藥劑之活性、個體之年齡、體重、一般健康狀況、性別及飲食、投藥時間、投藥途徑、排泄速率、及任何藥物組合(若適用)、專業人員希望化合物對個體之作用及化合物之特性(例如,生物可用性、穩定性、效能、毒性等),以及個體所罹患之特定病症。另外,經靜脈內投予之治療有效量可取決於個體之血液參數,例如脂質概況、胰島素含量、血糖或肝臟代謝。治療有效量亦將根據疾病狀態之嚴重程度、器官功能或潛在之疾病或併發症而改變。可使用任何可用之檢定(包括本文所述之檢定)來確定此等適當劑量。當一或多種本發明化合物欲投予人類時,醫師可例如首先規定相對低之劑量,隨後增大劑量直至獲得適當的反應。在人類中,根據本發明之化合物在人類中之經口投予劑量為1mg/kg至50mg/kg、較佳5mg/kg至20mg/kg、更佳5mg/kg至15mg/kg、此外更佳約1mg/kg至10mg/kg。本發明化合物在人類中之局部投予劑量為0.01%至10%(w/w)、較佳0.1%至5%(w/w)且更佳1%至5%。小鼠代謝比人類代謝更快地消除任何化合物,因此對於化合物於小鼠中之測試,劑量可倍增10倍至20倍。
如本文所用,術語「醫藥組成物」係指存在至少一種根據本發明之化合物及醫藥學上可接受之媒劑。
「醫藥學上可接受之媒劑」係指與化合物一起投予之稀釋劑、佐劑、賦形劑或載劑。術語「醫藥學上可接受」係指適用於與人類及低等動物之組織接觸而無不當毒性、不相容性、不穩定性、刺激性、過敏反應及其類似特性且與合理的效益/風險比相稱的藥物、藥劑、惰性成分等。其較佳係指已由或可由聯邦或州政府之管理機構批准或列於美國藥典或其他公認藥典中用於動物且更特定言之用於人類的化合物或組成物。醫藥學
上可接受之媒劑可為溶劑或分散介質,其包含例如水、乙醇、多元醇(例如甘油、丙二醇及液體聚乙二醇)、其合適混合物以及植物油。醫藥學上可接受之媒劑的其他實例包括但不限於:注射用水USP;水性媒劑,諸如但不限於氯化鈉注射液、林格氏注射液、右旋糖注射液、右旋糖/氯化鈉注射液及乳酸化林格氏注射液;水可混溶性媒劑,諸如但不限於乙醇、聚乙二醇及聚丙二醇;及非水性媒劑,諸如但不限於玉米油、棉籽油、花生油、芝麻油、油酸乙酯、肉豆蔻酸異丙酯及苯甲酸苄酯。可藉由添加抗細菌劑及抗真菌劑(例如對羥基苯甲酸酯、氯丁醇、苯酚、抗壞血酸、硫柳汞及其類似物)來達成微生物作用之預防。在許多情況下,組成物中包括等滲劑,例如糖、氯化鈉或多元醇諸如甘露糖醇及山梨糖醇。可藉由在組成物中包括延遲吸收劑(例如單硬脂酸鋁或明膠)來產生可注射組成物之延長吸收。
在一些實施方案中,本發明組成物包含有效量之具有上文式之化合物。尤其較佳為3-戊基苯基乙酸、3-羥基-5-戊基苯基乙酸及3-氟-5-戊基苯基乙酸之鈉鹽。
在一些實施方案中,本發明關於用於預防及/或治療肺纖維化、肝纖維化、心臟纖維化及皮膚纖維化之醫藥組成物。
本發明化合物可在投予之前使用可用技術及程序調配成醫藥組成物。例如,可以適於藉由局部、經口、靜脈內(iv)、肌肉內(im)、儲槽式肌肉內(depo-im)、皮下(sc)、儲槽式皮下(depo-sc)、舌下、鼻內、鞘內局部或直腸途徑投予的方式調配醫藥組成物。
較佳地,本發明化合物可經口投予或局部投予。調配物宜以單位劑型呈現且可藉由製藥技術中熟知之任何方法製備。製備此等調配物或組成物之方法包括使本發明化合物與醫藥學上可接受之媒劑(例如,惰性稀釋劑或可同化之食用載劑)及視情況一或多種輔助成分締合的步驟。一般而言,藉由使本發明化合物與液體載劑或細粉狀固體載劑或兩者均勻且緊密地締合以及隨後必要時成形產品來製備調配物。此等治療上有用之組成物中之治療劑的量使得可獲得合適劑量。
適於經口投予之本發明調配物可呈以下形式:膠囊(例如
硬殼或軟殼明膠膠囊)、扁囊劑、丸劑、錠劑、口含錠、散劑、顆粒劑、錠片、糖衣丸(例如有包衣(例如腸溶包衣)或無包衣),或於水性或非水性液體中之溶液或懸浮液,或水包油或油包水乳液,或酏劑或糖漿,或片劑或漱口劑以及其類似形式,其各含有預定量之本發明化合物作為活性成分。本發明化合物亦可以大丸劑、舐劑或糊劑形式投予,或直接併入個體之飲食中。此外,在某些實施方案中,此等錠片可經調配以(a)提供暫態或快速藥物釋放(亦即其上面無塗層);(b)經包覆例如以隨時間提供持續藥物釋放;或(c)包覆腸溶包衣以提供更好胃腸耐受性。可藉由習知方法達成包衣包覆,典型地為pH或時間依賴性包衣,以使得本發明化合物於所需位置附近釋放,或在多個時間釋放以延長所需作用。此等劑型典型地包括但不限於鄰苯二甲酸乙酸纖維素、聚乙酸乙烯酯鄰苯二甲酸酯、鄰苯二甲酸羥丙基甲基纖維素、乙基纖維素、蠟及蟲膠中之一或多者。
在用於經口投予之固體劑型中,本發明化合物可與一或多種醫藥學上可接受之載劑混合,諸如檸檬酸鈉或磷酸二鈣,或下列中之任一者:填充劑或增量劑,諸如澱粉、乳糖、蔗糖、葡萄糖、甘露糖醇或矽酸;黏合劑,例如羧甲基纖維素、海藻酸鹽、明膠、聚乙烯吡咯啶酮、蔗糖或阿拉伯膠;保濕劑,諸如甘油;崩解劑,諸如瓊脂、碳酸鈣、馬鈴薯或木薯澱粉、海藻酸、某些矽酸鹽及碳酸鈉;溶解阻滯劑,諸如石蠟;吸收促進劑,諸如四級銨化合物;濕潤劑,例如鯨蠟醇及單硬脂酸甘油酯;吸收劑,諸如高嶺土及膨潤土;潤滑劑,諸如滑石、硬脂酸鈣、硬脂酸鎂、固體聚乙二醇、月桂基硫酸鈉及其混合物;以及著色劑。在膠囊、錠劑及丸劑之情況下,醫藥組成物亦可包含緩衝劑。相似類型之固體組成物亦可用作使用諸如乳糖或奶糖以及高分子量聚乙二醇及其類似物之賦形劑之軟填充明膠膠囊及硬填充明膠膠囊中的填充劑。
經口組成物典型地包括液體溶液、乳液、懸浮液及其類似物。適於製備此等組成物之醫藥學上可接受之媒劑為本領域中所熟知。用於糖漿、酏劑、乳液及懸浮液之典型載劑組分包括乙醇、甘油、丙二醇、聚乙二醇、液體蔗糖、山梨糖醇及水。對於懸浮液而言,典型的懸浮劑包括甲基纖維素、羧甲基纖維素鈉、黃蓍膠及海藻酸鈉;典型的濕潤劑包括
卵磷脂及聚山梨醇酯80;且典型的防腐劑包括對羥基苯甲酸甲酯及苯甲酸鈉。經口液體組成物亦可含有一或多種組分,諸如上文揭示之甜味劑、調味劑及著色劑。
適於注射用途之醫藥製劑可包括無菌水溶液(具水溶性時)或分散液及用於臨時製備無菌可注射溶液或分散液之無菌粉末。在所有情況下,組成物必須無菌且必須為流體以便存在易注射性。其在製造及儲存條件下必須穩定且必須抵抗諸如細菌及真菌之微生物的污染作用。可藉由將所需量之治療劑與所需要之上文所列成分中之一者或組合併入適當溶劑中,接著過濾滅菌來製備無菌可注射溶液。一般而言,藉由將治療劑併入含有基本分散介質及來自上文所列成分之所需其他成分的無菌媒劑中來製備分散液。在用於製備無菌可注射溶液之無菌粉末之情況下,製備方法為真空乾燥及冷凍乾燥,其得到活性成分(亦即治療劑)加來自其先前無菌過濾溶液之任何額外所需成分的粉末。
亦提供適於以氣霧劑形式藉由吸入投予之醫藥調配物。此等調配物包含具有任何本文式之所需化合物或此(等)化合物之複數個固體粒子的溶液或懸浮液。例如,預期本發明化合物之金屬鹽具有可用於製備用於藉由吸入投予之活性醫藥成分(API)之精細粒子而非此等化合物之自由酸形式的物理化學特性。所需調配物可置於小腔中且噴霧。可藉由壓縮空氣或藉由超音能量來實現噴霧以形成複數個包含藥劑或鹽之液滴或固體粒子。該等液滴或固體粒子應具有約0.5至約5微米範圍內之粒徑。可藉由以本領域中已知之任何適當方式、諸如藉由微米尺寸化加工具有任何本文所述式之固體劑或其鹽來獲得固體粒子。固體粒子或液滴之尺寸應為例如約1至約2微米。在此方面,商業噴霧器可用于達成此目的。適於以氣霧劑形式投予之醫藥調配物可為液體形式,該調配物應于包含水之載劑中包含具有任何本文所述式之水溶性劑或其鹽。可存在介面活性劑,當進行噴霧時,該介面活性劑充分降低調配物之表面張力以導致形成在所需尺寸範圍內之液滴。
本發明組成物亦可經局部投予個體,例如,藉由將組成物直接放置於個體之表皮或上皮組織上或使組成物在個體之表皮或上皮組織上
擴散,或經由「貼片」經皮投予。此等組成物包括例如洗劑、乳膏、溶液、凝膠、乳液及固體。此等局部組成物可包含有效量、通常約0.01%至約10%(w/w)、或約0.1%至約5%(w/w)、或約1%至約5%(w/w)的本發明化合物。適於局部投予之載劑典型地以連續膜形式原位保留於皮膚上,且抵抗因排汗或浸于水中而移除。一般而言,載劑為有機性質且能夠於其中分散或溶解治療劑。該載劑可包括醫藥學上可接受之潤膚劑、乳化劑、增稠劑、溶劑及其類似物。載劑可包括胎脂。局部調配物包括一或多種賦形劑,諸如但不限於保護劑、吸附劑、緩和劑、潤膚劑、防腐劑、抗氧化劑、保濕劑、緩衝劑、增溶劑、皮膚滲透劑及介面活性劑。合適的保護劑及吸附劑包括但不限於粉塵劑、硬脂酸鋅、火棉膠、二甲聚矽氧烷、聚矽氧、碳酸鋅、蘆薈凝膠及其他蘆薈產品、維生素E油、尿囊素(allatoin)、甘油、礦脂及氧化鋅。合適的緩和劑包括但不限於安息香、羥丙基纖維素、羥丙基甲基纖維素及聚乙烯醇。合適的潤膚劑包括但不限於動物及植物脂肪及油、肉豆蔻醇、明礬及乙酸鋁。合適的防腐劑包括但不限於四級銨化合物,諸如氯化苯甲烴銨、苄索氯銨、西曲溴銨(cetrimide)、地喹氯銨(dequalinium chloride)及氯化十六烷基吡錠;汞劑,諸如硝酸苯汞、乙酸苯汞及硫柳汞;醇劑,例如氯丁醇、苯乙醇及苯甲醇;抗細菌酯,例如對羥基苯甲酸酯;及其他抗微生物劑,諸如氯己定(chlorhexidine)、氯甲酚、苯甲酸及多黏菌素。合適的抗氧化劑包括但不限於抗壞血酸及其酯、亞硫酸氫鈉、丁基化羥基甲苯、丁基化羥基苯甲醚、生育酚,及螯合劑如EDTA及檸檬酸。合適的保濕劑包括但不限於甘油、山梨糖醇、聚乙二醇、尿素及丙二醇。適於本發明使用之緩衝劑包括但不限於乙酸鹽緩衝劑、檸檬酸鹽緩衝劑、磷酸鹽緩衝劑、乳酸緩衝劑及硼酸鹽緩衝劑。合適的增溶劑包括但不限於四級銨氯化物、環糊精、苯甲酸苄酯、卵磷脂及聚山梨醇酯。合適的皮膚滲透劑包括但不限於乙醇、異丙醇、辛基苯基聚乙二醇、油酸、聚乙二醇400、丙二醇、N-癸基甲基亞碸、脂肪酸酯(例如,肉豆蔻酸異丙酯、月桂酸甲酯、單油酸甘油酯及丙二醇單油酸酯);及N-甲基吡咯啶酮。
可用於獲得藥劑於個體中之全身性傳遞的其他組成物可包括舌下、經頰及經鼻劑型。此等組成物典型地包含一或多種可溶性填充劑
物質,諸如蔗糖、山梨糖醇及甘露糖醇;及黏合劑,諸如阿拉伯膠、微晶纖維素、羧甲基纖維素及羥丙基甲基纖維素。亦可包括上文揭示之助流劑、潤滑劑、甜味劑、著色劑、抗氧化劑及調味劑。
根據本發明之化合物亦可非經腸、經腹膜內、經脊柱內或經腦內投予。對於此等組成物,本發明化合物可於甘油、液體聚乙二醇及其混合物中以及於油中製備。在普通儲存及使用條件下,此製劑可含有防腐劑以防止微生物之生長。
對於預防肺纖維化、肝纖維化、心臟纖維化或皮膚纖維化/減緩肺纖維化、肝纖維化、心臟纖維化或皮膚纖維化之進展/治療肺纖維化、肝纖維化、心臟纖維化或皮膚纖維化之方法,本發明之方法亦可包括共同投予至少一種根據本發明之化合物或其醫藥學上可接受之鹽以及投予另一治療有效劑用於預防肺纖維化、肝纖維化、心臟纖維化或皮膚纖維化及/或減緩肺纖維化、肝纖維化、心臟纖維化或皮膚纖維化之進展及/或治療肺纖維化、肝纖維化、心臟纖維化或皮膚纖維化。因此,本發明亦關於一種用於預防、減少或消除上述疾病或病狀中之任一者之症狀或併發症的方法。該方法包括向有需要之個體投予本發明化合物、包含至少一種本發明化合物之第一醫藥化合物及包含一或多種其他活性成分之第二醫藥組成物,其中所有活性成分以足以抑制、降低或消除欲治療之疾病或病狀之一或多種症狀或併發症的量投予。在一個態樣中,第一醫藥組成物與第二醫藥組成物之投予短暫間隔至少約兩分鐘。第一藥劑較佳為式I化合物。第二藥劑可選自上文給出化合物之清單。
本發明不欲局限于本文所示之實施方案,但符合與本文公開之原理及新穎特徵一致的最廣泛範疇。
除非上下文另外明確指示,否則單數形式「一」及「該」包括相應的複數個提及物。
除非另外指示,否則本說明書及申請專利範圍中所用之所有表示成分量、反應條件、濃度、性質等之數目應理解為在所有情形下皆由術語「約」修飾。最起碼,每個數值參數應當至少按照所報導之有效數字的數目且藉由應用普通捨入技術理解。因此,除非相反指示,否則本說明
書及隨附申請專利範圍中所述之數值參數為近似值,其可能根據欲獲得之特性而改變。儘管闡述實施方案之寬泛範疇之數值範圍及參數為近似值,但特定實施例中闡述之數值盡可能精確地報導。然而,任何數值皆固有地含有由實驗、測試量測、統計分析及此類之變化而產生的某些誤差。
熟習此項技術者應僅使用常規實驗可認識到或能夠確定本文所述之具體程序、實施方案、申請專利範圍及實施例的眾多等效物。此等等效物視為在本發明之範疇內且由其隨附申請專利範圍所涵蓋。本發明由下列實施例進一步說明,該等實施例不應理解為進一步限制本發明。
實施例
下文闡述之實施例提供由式I涵蓋之某些代表性化合物之例示性製備方法。一些實施例提供某些代表性本發明化合物之例示性用途。亦提供用於檢定本發明化合物之功效的例示性方法。
實施例1:
用於製備3-戊基苯基乙酸之鈉鹽(化合物I)的實驗程序
儀器:
所有HPLC層析圖及質譜記錄於HP 1100 LC-MS Agilent儀器上,其中使用分析型C18管柱(250×4.6mm,5微米),以5分鐘內含0.01% TFA之50-99% CH3CN-H2O之梯度作為洗提劑且流速為2mL/min,或以3分鐘內含0.01% TFA之50-99% CH3CN-H2O之梯度作為洗提劑,接著3分鐘內等度洗提且流速為2mL/min。
化合物I:使用改良式薗頭(Sonogashira)程序合成:
步驟1:
在室溫下向3-溴苯基乙酸(5.02g,23.33mmol)於乙醇(100mL)中之溶液/懸浮液添加濃硫酸(1mL)。無色固體隨後在80℃下攪拌隔夜。在減壓下濃縮溶液。用乙酸乙酯(25mL)、水(25mL)稀釋殘餘物且分離兩層。用2×乙酸乙酯(25mL)及鹽水(20mL)萃取水性層。經合併之有機層用2×碳酸氫鈉飽和溶液(25mL)、鹽水(25mL)洗滌且經硫酸鈉脫水。溶液過濾後,將其蒸發至乾燥。此舉得到淺黃色油狀物(5.4g,95%)。1H-NMR(400MHz,CDCl3):δ 1.26(t,J=4.7Hz,3H),3.57(s,2H),4.15(Q,J=7.0及14.3Hz,2H),7.17-7.26(m,2H),7.38-7.44(m,1H),7.44(d,J=1.56Hz,1H)。
步驟2:
在密封管中用PdCl2(PPh3)2(26mg,0.037mmol;3莫耳%)及1-戊炔(367μl,3.72mmol)處理(3-溴苯基)乙酸乙酯(0.3g,1.24mmol)與水合氟化四丁銨(0.97g,3.72mmol)之混合物。該管在80℃下加熱2小時。該混合物用水處理且用乙醚萃取。有機萃取物經硫酸鈉脫水,過濾且真空蒸發,得到粗產物。利用以乙酸乙酯/己烷0:1至2:98洗提之BiotageTM 25M管柱(二氧化矽)純化,得到呈淺黃色油狀之(3-(戊炔-1-基)苯基)乙酸乙酯(0.23g,79%)。
步驟3:
在氮氣氛圍下向含[3-[戊炔-1-基]苯基]-乙酸乙酯(0.23g,0.98mmol)之乙醇(5mL)中添加Pd/碳(10%,25mg,10%w/w)。在室溫下在氫氣氛圍下劇烈攪拌混合物隔夜。過濾溶液且用乙醇(20mL)洗滌鈀/碳。用矽膠濃縮濾液。藉由使用10%己烷/乙酸乙酯之混合物的急驟層析純化粗產物。獲得透明油狀物(0.21g,90%)。
步驟4:
在0℃下向酯(0.2g,0.9mmol)於四氫呋喃(5mL)、甲醇(1.5mL)及水(1.5mL)中之溶液中添加氫氧化鋰(0.09g,3.6mmol)。
在室溫下攪拌反應混合物隔夜。過濾不溶物且在減壓下濃縮濾液。殘餘物隨後用2M鹽酸處理且用乙酸乙酯萃取。有機相經硫酸鈉脫水且在減壓下蒸發。利用以40%乙酸乙酯/己烷洗提之BiotageTM 40M管柱(二氧化矽)純化粗物質。此舉得到呈膠質固體狀之純(3-戊基苯基)乙酸(0.19g,99%)。1H NMR(400MHz,CD3OD):δ 0.90(t,J=7.0Hz,3H),1.28-1.38(m,4H),1.61(qt,J=7.6Hz,15.0Hz,2H),2.58(t,J=7.6Hz,2H),3.56(s,2H),7.07(m,3H),7.20(m,1H);LRMS(ESI):m/z 207(MH+);HPLC:4.3分鐘。
步驟5:
向經攪拌之酸(0.19g,0.82mmol)於乙醇(4mL)及水(1mL)中之溶液中添加碳酸氫鈉(0.07g,0.82mmol)。在室溫下攪拌反應混合物隔夜。蒸發溶劑且將白色膠質固體溶解于水中且將溶液凍幹。此舉得到呈白色固體狀之純(3-戊基苯基)乙酸之鈉鹽(0.17g,92%)。熔點110-112℃;1H NMR(400MHz,CD3OD):δ 0.89(t,J=6.8Hz,3H),1.28-1.37(m,4H),1.60(qt,J=7.4Hz,15.0Hz,2H),2.56(t,J=7.6Hz,2H),3.43(s,2H),6.96(m,1H),7.12(m,3H);LRMS(ESI):m/z 207((MH+);HPLC:4.3分鐘。
實施例2:
用於製備3-羥基-5-戊基苯基乙酸之鈉鹽(化合物II)的實驗程序
步驟1:
用碳酸鉀(2.4g,17.4mmol)、碘化鉀(383mg,2.31mmol)及苄基溴(1.5mL,12.7mmol)處理[3,5-二羥基苯基]乙酸甲酯(2.1g,11.5mmol)於丙酮(100mL)中之溶液,且在室溫下攪拌混合物隔夜。反應物用水稀釋且用二氯甲烷(×3)萃取。經合併之有機萃取物經硫酸鈉脫水且在真空中蒸發。利用以40%乙酸乙酯/己烷洗提之BiotageTM 40M管柱(二氧化矽)純化粗物質,得到[3-苄氧基-5-羥基苯基]乙酸甲酯(1.0g,33%)。1H NMR(400MHz,CDCl3):δ 7.32-7.42(m,5H),6.48(d,J=1.4Hz,1H),6.38-6.39(m,2H),4.99(s,2H),3.69(s,3H),3.53(s,2H)。
步驟2:
在0℃下用N-苯基-雙(三氟磺醯基)醯亞胺(1.40g,3.9mmol)處理苄基醚(1.04g,3.8mmol)於二氯甲烷(15mL)中之溶液,隨後緩慢添加三乙胺(0.6mL,4.1mmol)。反應物在0℃下攪拌1小時,隨後在室溫下攪拌1小時。反應混合物用水稀釋,隨後用乙醚(×2)萃取。經合併之有機萃取物用1M氫氧化鈉水溶液、水(×2)及飽和氯化鈉水溶液洗滌,隨後經硫酸鈉脫水,過濾且在真空中蒸發,得到粗產物。利用以25%乙酸乙酯/己烷洗提之BiotageTM 40M管柱(二氧化矽)純化,得到[3-苄氧基-5-三氟甲烷磺醯氧基苯基]乙酸甲酯(1.2g,79%)。1H NMR(400MHz,CDCl3):δ 7.36-7.46(m,5H),6.98(s,1H),6.97(s,1H),6.84(s,1H),5.06(s,2H),3.72(s,3H),3.63(s,2H)。
步驟3:
用三氟甲磺酸酯(1.2g,3.0mmol)於二甲氧基乙烷(5mL)中之溶液處理E-1-戊烯-1-基硼酸頻哪醇酯(E-1-penten-1-ylboronic acid pinacol easter)(0.8g,3.9mmol)於二甲氧基乙烷(5mL)中之溶液。用鈀0(0.7g,0.6mmol)及2M碳酸鈉水溶液(1.3mL,2.6mmol)處理溶液。混合物隨後在90℃下加熱3天。將反應物冷卻至室溫且經由矽藻土過濾。在真空中蒸發濾液,且利用以5%乙酸乙酯/己烷洗提之BiotageTM 25M管柱(二氧化矽)純化粗物質,得到[3-苄氧基-5-[戊-1-烯基]苯基]乙酸甲酯(0.4g,40%)。1H NMR(400MHz,CDCl3):δ 7.36-7.47(m,5H),6.90-6.92(m,2H),6.79(dd,J=2.0,2.0Hz,1H),6.35(d,J=15.9Hz,1H),6.24(dt,J=15.9,6.8Hz,1H),5.07(s,2H),3.70(s,3H),3.59(s,2H),2.20(td,J=7.4,6.8Hz,2H),1.51(dt,J=7.4Hz,2H),0.98(t,J=7.4Hz,3H)。
步驟4:
用1%鈀/碳(40mg)處理烯烴(0.4g,1.2mmol)於乙醇(13mL)中之溶液。在室溫下在1atm氫氣下攪拌混合物隔夜。將反應物過濾,在真空中蒸發且利用以15%乙酸乙酯/己烷洗提之BiotageTM 25S管柱(二氧化矽)純化,得到[3-羥基-5-戊基苯基]乙酸甲酯(0.3g,93%)。1H NMR(400MHz,CDCl3):δ 6.64(s,1H),6.58-6.60(m,2H),3.70(s,3H),3.55(s,2H),
2.51(t,J=7.7Hz,2H),1.55-1.59(m,2H),1.28-1.34(m,4H),0.88(t,J=7.0Hz,3H)。
步驟5:
用水(3mL)及氫氧化鋰(155mg,6.4mmol)處理酯(0.3g,1.3mmol)於乙醇(12mL)中之溶液,且在室溫下劇烈攪拌混合物隔夜。反應混合物以水(100mL)稀釋;用二氯甲烷洗滌;隨後用1M鹽酸水溶液酸化至pH 1且用二氯甲烷(×3)萃取。經合併之有機萃取物經硫酸鈉(0.3g,95%)脫水。此物質不經進一步純化即使用。1H NMR(400MHz,CDCl3):δ 6.66(s,1H),6.58-6.59(m,2H),3.55(s,2H),2.52(t,J=7.7Hz,2H),1.55-1.59(m,2H)。
步驟6:
用碳酸氫鈉(0.1g,1.2mmol)處理酸(0.27g,1.23mmol)於乙醇(6mL)及水(6mL)中之溶液,且在室溫下攪拌反應物幾小時。在真空中濃縮溶劑,且將溶液以水稀釋,過濾(0.2μm)且凍幹,得到呈白色固體狀之[3-羥基-5-戊基苯基]乙酸鈉(0.3g,95%)。熔點63-66℃;1H NMR(400MHz,CD3OD):δ 6.63(s,1H),6.58(s,1H),6.42(s,1H),3.36(s,2H),2.48(t,J=7.6Hz,2H),1.55-1.62(m,2H),1.26-1.38(m,4H),0.89(t,J=6.8Hz,3H);13C NMR(101MHz,CD3OD):δ 177.79,155.31,142.36,137.62,119.08,111.66,111.18,43.70,34.17,29.95,29.56,20.87,11.64;LRMS(ESI):m/z 445.2(2M-2Na++3H+),m/z 223(M-Na++2H+);HPLC:3.5分鐘。
實施例3:
用於製備3-氟-5-戊基苯基乙酸之鈉鹽(化合物III)的實驗程序
步驟1:
在0℃下在氮氣下經12分鐘用硼烷-四氫呋喃複合物(1M,15mL,15mmol)以小量分批處理3-溴-5-氟苯甲酸(2.74g,12.5mmol)於四氫呋喃(6mL)中之溶液,隨後反應物在0℃下攪拌70分鐘,且在室溫下攪拌22小時。藉由添加甲醇(10mL)中止反應,且甲醇混合物在室溫下攪拌3小時,隨後在真空中蒸發(自甲醇中共蒸發,隨後自乙酸乙酯中蒸發),得到粗產物。將該物質溶解於乙酸乙酯(200mL)中,且用0.5M氫氧化鈉水溶液(200mL)及飽和氯化鈉水溶液(100mL)洗滌溶液;隨後經硫酸鈉脫水;過濾且在真空中蒸發,得到3-溴-5-氟苯甲醇(1.79g,67%)。1H NMR(400MHz,CDCl3):δ 7.29(s,1H),7.15(ddd,J HF=8.2Hz,J HH=2.2,1.8Hz,1H),7.00-7.02及7.02-7.04(dm,J HF=9.2Hz,J HH=未解析,1H),4.66(s,2H),2.04(br s,1H);19F NMR(377MHz,CDCl3):δ -111.05(dd,J HF=9.3,8.0Hz,1F);13C NMR(101MHz,CDCl3):δ 162.87(d,J CF=250.6Hz),145.42(d,J CF=6.9Hz),125.45(d,J CF=3.1Hz),122.69(d,J CF=9.2Hz),118.01(d,J CF=24.6Hz),112.51(d,J CF=21.5Hz),63.60(d,J CF=2.3Hz)。
步驟2:
經10分鐘用四溴化碳(3.34g,10.10mmol)以小量分批處理3-溴-5-氟苯甲醇(1.79g,8.39mmol)及三苯基膦(3.65g,10.10mmol)於二氯甲烷(45mL)中之溶液,隨後在室溫下攪拌反應物隔夜。在真空中
蒸發溶劑,且用乙醚(50mL)處理殘餘物。在室溫下攪拌所得白色漿液,隨後經由矽藻土過濾。用乙醚(2×50mL)洗滌殘餘物,且在真空中蒸發組合之濾液及洗滌液,得到粗產物。利用以2%乙酸乙酯/己烷洗提之二氧化矽墊純化,得到3-溴-5-氟苄基溴(2.21g,98%)。1H NMR(400MHz,CDCl3):δ 7.33(s,1H),7.18(ddd,J HF=8.2Hz,J HH=2.0,2.0Hz,1H),7.05(ddd,J HF=9.0Hz,J HH=1.8,1.6Hz,1H),4.38(s,2H);19F NMR(377MHz,CDCl3):δ -110.19至-110.14(m,1F);13C NMR(101MHz,CDCl3):δ 162.67(d,J CF=252.1Hz),141.61(d,J CF=8.5Hz),128.17(d,J CF=3.1Hz),122.94(d,J CF=10.0Hz),119.39(d,J CF=24.6Hz),115.34(d,J CF=22.3Hz),31.31(d,J CF=2.3Hz)。
步驟3:
用3-溴-5-氟苄基溴(1.38g,5.15mmol)於二甲基甲醯胺(2.6mL)中之溶液處理氫化鈉(0.38g,7.73mmol)于水(0.35mL)中之懸浮液,且反應物在密封管中在75℃下加熱3小時。將反應物冷卻至室溫且分配於乙酸乙酯(50mL)與2.5% w/v碳酸氫鈉水溶液(100mL)之間。用另一部分乙酸乙酯(50mL)萃取水相;且經合併之萃取物用水(2×50mL)及飽和氯化鈉水溶液(50mL)洗滌,經硫酸鈉脫水,過濾,且在真空中蒸發,得到粗產物。利用以10%乙酸乙酯/己烷洗提之BiotageTM 40iM管柱(二氧化矽)純化,得到2-[3-溴-5-氟苯基]乙腈(0.64g,58%)。1H NMR(400MHz,CDCl3):δ 7.26-7.28(m,1H),7.17-7.19及7.19-7.21(dm,J HF=8.0Hz,J HH=未解析,1H),6.98-7.00及7.00-7.02(dm,J HF=8.8Hz,J HH=未解析,1H),3.73(s,2H);19F NMR(377MHz,CDCl3):δ -109.46(dd,J HF=8.0,8.0Hz,1F);13C NMR(101MHz,CDCl3):δ 162.90(d,J CF=252.1Hz),133.95(d,J CF=8.5Hz),127.24(d,J CF=3.8Hz),123.53(d,J CF=10.0Hz),119.22(d,J CF=23.8Hz),117.00,114.50(d,J CF=23.1Hz),23.30(d,J CF=1.5Hz)。
步驟4:
用碳酸鈉(0.55g,5.17mmol)于水(3mL)中之溶液處理芳基溴(0.55g,2.58mmol)及(E)-1-戊烯-1-基硼酸頻哪醇酯(0.61g,3.13
mmol)於二甲氧基乙烷(13mL)中之溶液。用氮氣使溶液去氧,且用肆(三苯基膦)鈀(0.15g,0.13mmol;5莫耳%)處理。隨後混合物于密封管中在90℃下加熱17小時。將反應物冷卻至室溫且分配於乙酸乙酯(50mL)與1M鹽酸水溶液(50mL)之間。有機相以飽和氯化鈉水溶液(30mL)洗滌,經硫酸鈉脫水,過濾且在真空中蒸發,得到粗產物。利用以(3%)乙酸乙酯/己烷洗提之BiotageTM 40iM管柱(二氧化矽)純化,得到(E)-2-[3-氟-5-[戊-1-烯基]苯基]乙腈(0.43g,82%)。1H NMR(400MHz,CDCl3):δ 7.04(s,1H),6.97(ddd,J HF=9.8Hz,J HH=2.0,1.5Hz,1H),6.82-6.85(m,1H),6.31(d,J=15.8Hz,1H),6.25(ddd,J=15.8,5.9,0Hz,1H),3.68(s,2H),2.18(td,J=7.2,5.4Hz,2H),1.49(qt,J=7.4,7.4Hz,2H),0.95(t,J=7.4Hz,3H);19F NMR(377MHz,CDCl3):δ -112.93(dd,J HF=10.6,9.3Hz,1F);13C NMR(101MHz,CDCl3):δ 163.43(d,J CF=246.0Hz),141.44(d,J CF=8.5Hz),133.99,132.37(d,J CF=8.5Hz),128.42(d,J CF=2.3Hz),121.60(d,J CF=3.1Hz),117.66,113.40(d,J CF=23.1Hz),112.21(d,J CF=22.3Hz),35.22,23.49(d,J CF=2.3Hz),22.51,13.94。
步驟5:
用氫氧化鈉水溶液(5M;21mL,105mmol)處理苯基乙腈衍生物(0.43g,2.10mmol)於甲醇(42mL)中之溶液,且混合物于密封管中在75℃下加熱4.5小時。將反應混合物冷卻至室溫,且用6M鹽酸水溶液(21mL)中止;在室溫下攪拌10分鐘;隨後用乙酸乙酯(2×75mL)萃取。有機萃取物以飽和氯化鈉水溶液(75mL)洗滌;經硫酸鈉脫水;過濾,且在真空中蒸發,得到粗產物。利用以70%乙酸乙酯/己烷洗提之BiotageTM 40iM管柱(二氧化矽)純化,得到所需產物之甲酯(0.09g,18%),及約95%純度之(E)-2-[3-氟-5-[戊-1-烯基]苯基]乙酸(0.22g,48%)。1H NMR(400MHz,CDCl3):δ 11.17(br s,1H),7.02(s,1H),6.98(ddd,J HF=9.8Hz,J HH=2.0,1.8Hz,1H),6.85(ddd,J HF=9.0Hz,J HH=1.8,1.6Hz,1H),6.33(d,J=15.8Hz,1H),6.25(dt,J=15.8,6.4Hz,1H),3.62(s,2H),2.17-2.22(m,2H),1.51(qt,J=7.4,7.4Hz,2H),0.96(t,J=7.4Hz,3H);19F NMR(377MHz,
CDCl3):δ -114.10(dd,J HF=9.3,9.3Hz,1F)。
步驟6:
用碳酸鉀(0.26g,1.90mmol)、碘化鉀(0.04g,0.25mmol)及苄基溴(0.18mL,1.5mmol)處理部分純化之酸(0.28g,1.26mmol)於丙酮(5mL)中之溶液,且在室溫下攪拌反應物18小時。反應混合物分配於乙酸乙酯(25mL)與1M鹽酸水溶液(25mL)之間。有機相隨後用飽和氯化鈉水溶液(25mL)洗滌;經硫酸鈉脫水,過濾,且在真空中蒸發,得到粗產物。利用以5%乙酸乙酯/己烷洗提之BiotageTM 40iM管柱(二氧化矽)純化,得到(E)-2-[3-氟-5-[戊-1-烯基]苯基]乙酸苄酯(0.3g,75%)。1H NMR(400MHz,CDCl3):δ 7.32-7.40(m,5H),7.03(s,1H),6.97(ddd,J HF=10.0Hz,J HH=2.3,1.5Hz,1H),6.86(ddd,J HF=9.0Hz,J HH=2.0,1.7Hz,1H),6.33(d,J=15.8Hz,1H),6.23(dt,J=15.8,6.5Hz,1H),5.16(s,2H),3.64(s,2H),2.17-2.23(m,2H),1.52(qt,J=7.4,7.4Hz,2H),0.97(t,J=7.4Hz,3H);19F NMR(377MHz,CDCl3):δ -114.34(dd,J HF=9.3,9.3Hz,1F);13C NMR(101MHz,CDCl3):δ 171.08,163.32(d,J CF=244.4Hz),140.65(d,J CF=7.7Hz),136.17(d,J CF=8.5Hz),135.93,133.05,128.95(d,J CF=3.1Hz),128.84,128.52(d,J CF=9.2Hz),128.48,123.09(d,J CF=2.3Hz),114.78(d,J CF=22.3Hz),111.46(d,J CF=22.3Hz),67.04,41.26(d,J CF=1.5Hz),35.27,22.63,14.00。
步驟7:
用鈀/碳(1% w/w Pd;15mg)處理苄基酯(0.16g,0.50mmol)於乙酸乙酯(2mL)中之溶液。用氫氣使混合物脫氣,且在室溫下在1atm氫氣下攪拌隔夜。將反應物過濾,且在真空中蒸發,得到2-[3-氟-5-戊基苯基]-乙酸(0.11g,97%)。1H NMR(400MHz,CDCl3):δ 11.47(br s,1H),6.89(s,1H),6.81-6.86(m,2H),3.62(s,2H),2.60(t,J=7.8Hz,2H),1.58-1.66(m,2H),1.28-1.41(m,4H),0.92(t,J=6.8Hz,3H);19F NMR(377MHz,CDCl3):δ -114.34(dd,J HF=9.3,9.3Hz,1F);13C NMR(101MHz,CDCl3):δ 178.15,163.08(d,J CF=246.0Hz),145.02(d,J CF=7.7Hz),135.04(d,J CF=8.5Hz),
125.49(d,J CF=2.3Hz),114.49(d,J CF=20.8Hz),113.83(d,J CF=22.3Hz),41.01(d,J CF=1.5Hz),35.87(d,J CF=1.5Hz),31.67,31.03,22.74,14.24。
步驟8:
用碳酸氫鈉(0.041g,0.49mmol)于水(0.75mL)中之溶液處理酸(0.11g,0.49mmol)於乙醇(3mL)中之溶液,且在室溫下攪拌反應物17小時。在真空中蒸發乙醇,且殘餘水性糖漿狀物用水(10mL)稀釋,過濾(0.2μm),且凍幹,得到呈白色固體狀之2-[3-氟-5-戊基苯基]乙酸鈉(0.12g,99%)。熔點120-123℃;1H NMR(400MHz,CD3OD):δ 6.94(s,1H),6.87(ddd,J HF=9.8Hz,J HH=2.0,2.0Hz,1H),6.70(ddd,J HF=10.0Hz,J HH=2.0,2.0Hz,1H),3.45(s,2H),2.56(t,J=7.7Hz,2H),1.58-1.63(m,2H),1.26-1.39(m,4H),0.90(t,J=7.0Hz,3H);19F NMR(377MHz,CD3OD):δ -117.54(dd,J HF=10.0,10.0Hz,1F);13C NMR(101MHz,CD3OD):δ 178.66,163.04(d,J CF=242.9Hz),145.07(d,J CF=7.7Hz),140.42(d,J CF=8.5Hz),125.03(d,J CF=2.3Hz),112.99(d,J CF=22.3Hz),112.30(d,J CF=20.8Hz),44.96,35.53(d,J CF=1.5Hz),31.46,31.00,22.45,13.30;HPLC:1.2分鐘。
實施例4:
化合物IV,E-(3-戊-1-烯基-苯基)乙酸之鈉鹽
如關於化合物I所述以E-(3-戊-1-烯基-苯基)乙酸甲酯為起始物質來製備上述化合物。藉由在鈴木條件(Suzuki condition)下使3-溴苯基乙酸甲酯與反-1-戊烯基硼酸頻哪醇酯反應來製備該化合物。白色固體;1H NMR(400MHz,CD3OD):δ=7.32(s,1H),7.11-7.18(m,3H),6.35(d,J=15.7Hz,1H),6.20-6.27(m,1H),3.44(s,2H),2.19(m,2H),1.45-1.54(m,2H),0.96(t,J=7.4,3H);13C NMR(101MHz,CD3OD):δ=179.26,138.25,137.92,130.32,130.04,128.06,127.59,126.60,123.52,45.21,35.06,22.52,12.89;LRMS(ESI):m/z 205(MH+);HPLC:4.1分鐘。
實施例5:
化合物V,(2-羥基-5-戊基苯基)乙酸之鈉鹽
如關於化合物I所述以5-溴-2-甲氧基苯基乙酸甲酯為起始物質來製備上述化合物。使用三溴化硼溶液(1M/CH2Cl2)在-78℃下進行甲氧基之脫甲基化進行1小時,隨後在0℃下進行20分鐘。白色固體;1H NMR(400MHz,CD3OD):δ=6.88(m,2H),6.71(d,J=8.6Hz,1H),3.50(s,2H),2.49(t,J=7.6Hz,2H),1.54-1.62(m,2H),1.29-1.38(m,4H),0.91(t,J=7.0Hz,3H);13C NMR(101MHz,CD3OD):δ=180.08,154.04,134.03,130.26,127.36,124.15,116.57,42.48,34.91,31.60,31.42,22.45,13.24;LRMS(ESI):m/z 177(MH+-CO-NaOH);HPLC:3.7分鐘。
實施例6:
化合物VI,3-(4-氟-3-戊基苯基)丙酸之鈉鹽
如關於化合物I所述以E-3-(3-溴-4-氟苯基)丙烯酸甲酯為起始物質來製備上述化合物。藉由在室溫下混合3-溴-4-氟苯甲醛及乙氧基羰基亞甲基三苯基磷烷于無水二氯甲烷中之溶液來製備該化合物。白色固體;1H NMR(400MHz,CD3OD):δ=6.67-6.74(m,2H),6.58(m,1H),2.49(t,J=7.6Hz,2H),2.23(t,J=7.4Hz,2H),2.15(m,2H),1.25(m,2H),0.99-1.06(m,4H),0.61(t,J=6.7Hz,3H);13C NMR(101MHz,D2O):δ=182.38,160.69,158.28,137.37,130.34,129.58,126.84,114.99,39.68,31.51,29.92,28.90,22.31,16.66;LRMS(ESI):m/z 221(MH+-H2O);HPLC:4.5分鐘。
實施例7:
化合物VII,3-(3-戊基苯基)丙酸之鈉鹽
如關於化合物I所述以3-側氧基-3-溴苯基丙酸乙酯為起始物質來製備上述化合物。在氫氣壓力下在乙醇中使用鈀/碳同時還原酮基及
雙鍵。白色固體;1H NMR(400MHz,CDCl3):δ 7.14-7.10(m,1H),7.04-7.00(m,2H),6.95-6.93(m,1H),2.88-2.84(m,2H),2.55(t,J=7.4Hz,2H),2.44-2.40(m,2H),1.63-1.55(m,2H),1.35-1.28(m,4H),0.90(m,3H);13C NMR(101MHz,CD3OD):δ 179.3,141.2,140.8,126.7,126.4,124.0,123.8,38.6,34.2,31.2,29.9,29.8,20.9,11.7;LRMS(ESI):m/z 203(MH+-CO-NaOH);HPLC:4.5分鐘。
實施例8:
化合物VIII,2-(3-戊基苯基)丙酸之鈉鹽
如關於化合物I所述以2-甲基-2-(3-戊基苯基)丙二酸二乙酯為起始物質來製備上述化合物。藉由使2-(3-溴苯基)丙二酸二乙酯與碘甲烷反應,接著使用反-1-戊烯基-1-硼酸頻哪醇酯進行鈴木偶合,隨後藉由氫化來還原雙鍵,以製備該化合物。白色固體;1H NMR(400MHz,CD3OD):δ 7.19-6.95(m,4H),3.54(q,J=7.0Hz,1H),2,56(t,J=7.6Hz,2H),1.64-1.56(m,2H),1.38(d,J=7.2Hz,3H),1.37-1.20(m,4H),0.90(t,J=7.0Hz,3H);13C NMR(CD3OD):δ 182.2,144.4,142.5,127.8,127.6,125.8,124.7,49.2,35.9,31.5,31.3,22.4,19.0,13.2;LRMS(ESI):m/z 221(M-Na++2H+);HPLC:4.5分鐘。
實施例9:
化合物IX,2-氟-2-(3-戊基苯基)乙酸之鈉鹽
如實施例1所述自2-氟-2-(3-戊基苯基)乙酸乙酯來製備上述化合物。藉由在-78℃下在四氫呋喃中使2-(3-戊基苯基)乙酸乙酯與二異丙胺基鋰及N-氟苯磺醯亞胺反應來製備該酯。白色固體;1H NMR(400MHz,CD3OD):δ 7.34(s,1H),7.30(dd,J=7.6,1.4Hz,1H),7.24(dd,J=7.6,7.6Hz,
1H),7.13(dd,J=7.4,1.0Hz,1H),5.53(d,J HF=51.3Hz,1H),2.60(t,J=7.7Hz,2H),1.59-1.65(m,2H),1.27-1.39(m,4H),0.76(t,J=6.9Hz,3H);13C NMR(101MHz,CD3OD):δ 173.73(d,J CF=23.9Hz),141.34,136.37(d,J CF=20.0Hz),126.79(d,J CF=2.3Hz),126.40,125.41(d,J CF=5.4Hz),122.84(d,J CF=5.4Hz),90.34(d,J CF=183.4Hz),34.13,29.91,29.65,20.85,11.64;19F NMR(377MHz,CD3OD):δ -168.83(d,J HF=51.7Hz,1F);LRMS(ESI負模式):m/z 223.0(100%,M-Na+);HPLC:4.1分鐘。
實施例10:
化合物X,2-甲基-2-(3-戊基苯基)丙酸之鈉鹽
步驟1:
將氫化鈉(60% w/w於礦物油中;0.5g,13.6mmol)于無水THF(8mL)中之懸浮液冷卻至0℃,且用[3-戊基苯基]乙酸甲酯(1.0g,4.5mmol)于無水THF(4mL)中之溶液處理。反應物在0℃下攪拌60分鐘,隨後用碘甲烷(0.7mL,11.3mmol)處理。使反應物緩慢地溫至室溫,且在此溫度下攪拌隔夜。藉由添加飽和氯化銨水溶液(10mL)中止反應,且用乙醚(3×20mL)萃取混合物。經合併之萃取物經硫酸鎂脫水且蒸發至乾燥。利用以乙酸乙酯/己烷1:99、然後2:98洗提之二氧化矽墊純化,得到呈無色油狀之2-甲基-2-(3-戊基苯基)丙酸甲酯(0.68g,60%)。1H NMR(400
MHz,CD3OD):δ 7.18-7.22(m,1H),7.08-7.13(m,2H),7.02-7.05(m,1H),3.62(s,3H),2.58(t,J=7.6Hz,2H),1.55-1.62(m,2H),1.53(s,6H),1.28-1.36(m,4H),0.90(t,J=7.1Hz,3H);HPLC:5.5分鐘。
步驟2:
用氫氧化鋰(0.2g,8.2mmol)處理酯於THF(8mL)、甲醇(2mL)及水(2mL)中之溶液,且反應物在室溫下攪拌隔夜,隨後在50℃下攪拌2天,且在室溫下攪拌10天。過濾反應物且用甲醇(2×20mL)洗滌漏斗。用2M鹽酸(7mL)處理經合併之濾液及洗滌液,且用乙酸乙酯(3×40mL)萃取混合物。經合併之萃取物以水(2×30mL)洗滌,經硫酸鈉脫水,過濾且在真空中蒸發,得到呈淺黃色糖漿狀之2-甲基-2-(3-戊基苯基)丙酸(0.64g,99%)。此物質不經進一步純化即使用。1H NMR(400MHz,CDCl3):δ 7.19-7.27(m,3H),7.07-7.10(m,1H),2.60(t,J=7.8Hz,2H),1.60(s,6H),1.58-1.63(m,2H),1.30-1.37(m,4H),0.89(t,J=7.0Hz,3H);LRMS(ESI):m/z 257(MNa+);HPLC:4.7分鐘。
步驟3:
用水(4mL)及碳酸氫鈉(0.2g,2.7mmol)處理酸於乙醇(16mL)中之溶液,且反應物在室溫下攪拌3天。在真空中蒸發溶劑,且將殘餘物溶解于水中,過濾且凍幹,得到呈白色固體狀之2-甲基-2-[3-戊基苯基]丙酸鈉(0.7g,96%)。1H NMR(400MHz,CD3OD):δ 7.19-7.23(m,2H),7.13(dd,J=7.6,7.6Hz,1H),6.91-6.95(m,1H),2.56(t,J=7.7Hz,2H),1.56-1.63(m,2H),1.46(s,6H),1.28-1.39(m,4H),0.90(t,J=7.0Hz,3H);13C NMR(101MHz,CD3OD):δ 184.35,148.62,142.13,127.51,126.14,125.32,123.16,36.01,31.57,31.40,27.45,22.44,13.22;LRMS(ESI):m/z 235;
(M-Na++2H+);HPLC:4.6分鐘。
實施例11:
化合物XI,2-(3-己基苯基)乙酸之鈉鹽
藉由如實施例2所述使2-(3-溴苯基)乙酸甲酯與(E)-己-1-烯基硼酸頻哪醇酯進行鈴木偶合;接著如實施例1所述進行氫化、酯水解及鈉鹽形成,來製備上述化合物。白色固體;1H NMR(400MHz,D2O):δ 7.14(dd,J=7.8,7.6Hz,1H),7.01(s,1H),7.00(d,J=7.8Hz,1H),6.96(d,J=7.6Hz,1H),3.34(s,2H),2.46(d,J=7.5Hz,2H),1.41-1.48(m,2H),1.10-1.18(m,6H),0.70(t,J=6.8Hz,3H);13C NMR(101MHz,D2O):δ 181.23,143.98,137.46,129.47,128.73,126.63,126.48,44.58,35.14,31.12,30.94,28.23,22.13,13.53;LRMS(ESI):m/z 265(100%,M+Na+);HPLC:4.6分鐘。
實施例12:
化合物XII,2-(3-(己-1-烯基]苯基)乙酸之鈉鹽
藉由如實施例2所述使2-(3-溴苯基)乙酸甲酯與(E)-己-1-烯基硼酸頻哪醇酯進行鈴木偶合;接著酯水解及鈉鹽形成,來製備上述化合物。白色固體;1H NMR(400M Hz,CD3OD):δ 7.33(s,1H),7.12-7.19(m,3H),6.35(d,J=15.8Hz,1H),6.20(dt,J=15.8,6.8Hz,1H),3.46(s,2H),2.17-2.22(m,2H),1.33-1.49(m,4H),0.93(t,J=7.2Hz,3H);13C NMR(101MHz,CD3OD):δ 179.35,138.27,137.95,130.27,130.16,128.10,127.61,126.64,123.56,45.24,32.66,31.67,22.16,13.22;LRMS(ESI):m/z 263(100%,M+Na+);HPLC:4.4分鐘。
實施例13:
化合物XIII,2-(2-氟-5-(戊-1-烯基)苯基)乙酸之鈉鹽
如實施例2所述自(E)-戊-1-烯基硼酸頻哪醇酯及2-(5-溴-2-氟苯基)乙酸乙酯來製備上述化合物。熔點215-220℃;白色固體;1H NMR(400MHz,D2O):δ 7.12-7.17(m,2H),6.90(dd,J HF=9.5Hz,J HH=9.5Hz,1H),6.28(d,J=16.0Hz,1H),6.15(dt,J=16.0,6.8Hz,1H),3.37(s,2H),2.00-2.05(m,2H),1.29-1.34(m,2H),0.76(t,J=7.4Hz,3H);13C NMR(101MHz,D2O):δ 180.02,160.30(d,J CF=243.5Hz),134.09(d,J CF=3.8Hz),131.99(d,J CF=1.5Hz),128.99(d,J CF=4.6Hz),128.49,125.84(d,J CF=7.7Hz),124.60(d,J CF=17.0Hz),115.44(d,J CF=21.6Hz),37.88(d,J CF=2.3Hz),34.56,22.03,13.13;19F NMR(377MHz,D2O):δ -121.11至-121.05(m,1F);LRMS(ESI):m/z 267(100%,M+Na+);HPLC:2.4分鐘。
實施例14:
化合物XIV,2-(4-羥基-3-戊基苯基)乙酸之鈉鹽
藉由如實施例2所述使2-(4-(苄氧基)-3-溴苯基)乙酸苄酯及(E)-戊-1-烯基硼酸頻哪醇酯進行鈴木偶合;接著氫化,來製備上述化合物。白色固體;熔點192-195℃;1H NMR(400MHz,CD3OD):δ 7.01(d,J=2.3Hz,1H),6.93(dd,J=8.2,2.3Hz,1H),6.64(d,J=8.2Hz,1H),3.35(s,2H),2.53(t,J=7.7Hz,2H),1.54-1.61(m,2H),1.30-1.37(m,4H),0.90(t,J=7.2Hz,3H);13C NMR(101MHz,CD3OD):δ 180.25,153.20,130.54,128.80,128.76,127.10,114.49,44.45,31.84,30.10,29.73,22.52,13.31;LRMS(ESI):m/z 245.2(55%,MH+),177.4(100%,M-CO2Na);HPLC:1.9分鐘。
實施例15:
化合物XV,2-(4-氟-3-戊基苯基)乙酸之鈉鹽
藉由如實施例3(步驟4)所述之鈴木偶合自2-(3-溴-4-氟苯
基)乙酸甲酯起始;接著如實施例1(步驟3、4及5)所述進行氫化、酯水解及鹽形成來製備上述化合物。藉由在硫酸存在下使2-(3-溴-4-氟苯基)乙酸與甲醇反應來製備起始酯。白色固體;1H NMR(400MHz,CD3OD):δ 7.16(dd,J HF=7.4Hz,J HH=2.3Hz,2H),7.08(ddd,J HF=5.0Hz,J HH=8.3,2.3Hz,1H),6.88(dd,J HF=10.1Hz,J HH=8.3Hz,1H),3.40(s,2H),2.59(t,J=7.7Hz,2H),1.55-1.63(m,2H),1.28-1.40(m,4H),0.90(t,J=7.0Hz,3H);13C NMR(101MHz,CD3OD):δ 179.12,159.88(d,J CF=240.6Hz),133.88(d,J CF=3.8Hz),131.26(d,J CF=4.6Hz),128.78(d,J CF=16.1Hz),127.96(d,J CF=8.5Hz),114.26(d,J CF=23.1Hz),44.38,31.51,30.00,28.76(d,J CF=1.5Hz),22.36,13.18;19F NMR(377MHz,CD3OD):δ -126.45至-126.40(m,1F);LRMS(ESI):m/z 225.2(M-Na++2H+);HPLC:1.9分鐘。
實施例16:
化合物XVI,2-(2-氟-3-戊基苯基)乙酸之鈉鹽
如關於化合物III所述,以3-溴-2-氟苯甲酸為起始物質來製備上述化合物。白色固體;1H NMR(400MHz,CD3OD):δ 7.13(ddd,J HF=7.0Hz,J HH=7.4,1.9Hz,2H),7.03(ddd,J HF=7.0Hz,J HH=7.4,1.9Hz,1H),6.97(dd,J HH=7.4,7.4Hz,1H),3.51(d,J HF=1.4Hz,2H),2.61(t,J=7.6Hz,2H),1.56-1.63(m,2H),1.28-1.40(m,4H),0.90(t,J=6.9Hz,3H);13C NMR(101MHz,CD3OD):δ 178.21,159.70(d,J CF=242.9Hz),129.07(d,J CF=4.6Hz),128.88,128.43(d,J CF=5.4Hz),125.02(d,J CF=17.7Hz),123.31(d,J CF=4.6Hz),37.89(d,J CF=3.8Hz),31.55,29.98,28.91(d,J CF=3.1Hz),22.41,13.26;19F NMR(377MHz,CD3OD):δ -126.09至-126.05(m,1F);LRMS(ESI):m/z 220.0(M-CO2Na+乙腈),179.4(M-CO2Na);HPLC:1.2分鐘。
實施例17:
化合物XVII,3-(4-羥基-3-戊基苯基)丙酸之鈉鹽
藉由如實施例3(步驟4)所述之鈴木偶合自3-(4-苄氧基-3-溴苯基)丙酸甲酯起始;接著如實施例1(步驟3、4及5)所述進行氫化、酯水解及鹽形成來製備上述化合物。藉由在碳酸鈉存在下使3-(4-苄氧基-3-溴苯基)丙酸與碘甲烷于丙酮/水中反應來製備起始酯。棕褐色固體;1H NMR(400MHz,CD3OD):δ 7.34(s,1H),6.90(d,J=2.2Hz,1H),6.84(dd,J=8.0,2.2Hz,1H),6.61(d,J=8.0Hz,1H),2.75-2.79(m,2H),2.52(t,J=7.8Hz,2H),2.35-2.39(m,2H),1.52-1.60(m,2H),1.28-1.41(m,4H),0.90(t,J=7.0Hz,3H);13C NMR(101MHz,CD3OD):δ 181.15,152.90,133.23,129.71,128.86,126.10,114.57,40.56,32.06,31.79,30.06,29.71,22.48,13.27;LRMS(ESI負模式):m/z 235.3(M-Na+);UPLC(系統A):5.2分鐘。UPLC系統A:移動相A=10mM碳酸氫銨水溶液;移動相B=水;固定相=HSS T3管柱;梯度=含5-100% B之A,經10分鐘。
實施例18:
化合物XVIII,2-側氧基-2-(3-戊基苯基)乙酸之鈉鹽
步驟1
在氮氣下將2-(3-甲基苯基)-2-側氧基乙酸乙酯(1.06g,5.5mmol)及偶氮雙異丁腈(9mg,0.06mmol)於乙腈(3ml)中之溶液加熱至80℃,且經60分鐘用N-溴代丁二醯亞胺(1.17g,6.6mmol)及偶氮雙異丁腈(9mg,0.06mmol)於乙腈(6ml)中之溶液逐滴處理。反應物在80℃下攪拌30分鐘;添加另一份偶氮雙異丁腈(9mg,0.06mmol);且在60℃下攪拌混合物21.5小時。將混合物冷卻至室溫且用乙酸乙酯(50ml)稀釋。溶液以水(2×50ml)及飽和氯化鈉水溶液(50ml)洗滌;隨後經硫酸鈉脫水;過濾且在真空中蒸發,得到粗產物。利用以含0-10%乙酸乙酯之己烷洗提之BiotageTM SP1系統(120g二氧化矽濾筒)純化,得到2-(3-(溴甲基)苯基)-2-側氧基乙酸乙酯(1.30g,95%)。1H NMR(400MHz,CDCl3):δ 7.96-7.97(m,1H),7.84-7.87(m,1H),7.60-7.62(m,1H),7.41(dd,J=7.7,7.7Hz,1H),4.45(s,2H),4.39(q,J=7.2Hz,2H),1.34(t,J=7.2Hz,3H)。
步驟2
在氬氣下將2-(3-(溴甲基)苯基)-2-側氧基乙酸乙酯(0.27g,1.0mmol)及2-溴乙醇(0.19g,1.5mmol)於N,N-二甲基甲醯胺(0.7ml)及四氫呋喃(0.5ml)中之溶液冷卻至-60℃,且經30分鐘逐滴添加N,N-二甲基甲醯胺(0.3ml)及第三丁醇鉀溶液(1M於四氫呋喃中;1.5ml)之混合物。反應物在-60℃下再攪拌95分鐘,隨後藉由添加飽和氯化銨水溶液(3ml)中止。在溫至室溫後,反應混合物以水(10ml)及飽和氯化鈉水溶液(10ml)稀釋,隨後用乙酸乙酯(5×10ml)萃取。經合併之有機萃取物以飽和氯化鈉水溶液(3×10ml)洗滌;隨後經硫酸鈉脫水;過濾且在真空中蒸發,得到粗產物。利用以含0-10%乙酸乙酯之己烷洗提之BiotageTM SP1系統(25g二氧化矽濾筒)純化,得到2-(3-(溴甲基)苯基)-1,3-二氧雜環戊烷-2-甲酸乙酯(0.17g,68%)。1H NMR(400MHz,CDCl3):δ 7.62(dd,J=1.6,1.6Hz,1H),7.52(dd,J=7.4,1.6Hz,1H),7.39(dd,J=7.8,1.6Hz,1H),7.33(dd,J=7.8,7.4Hz,1H),4.47(s,2H),4.19(q,J=7.1Hz,2H),4.15-4.20(m,2H),4.05-4.09(m,2H),1.22(t,J=7.1Hz,3H)。
步驟3
在氮氣下在-10℃下經5分鐘逐滴添加正丁基鋰溶液(2.5M於己烷中;0.53ml;1.3mmol)至碘化銅(I)(0.13g,0.66mmol)於環戊基甲醚(2.6ml)中之懸浮液。深綠色混合物在-10℃下攪拌15分鐘;隨後冷卻至-40℃;且經10分鐘用2-(3-(溴甲基)苯基)-1,3-二氧雜環戊烷-2-甲酸酯(0.17g,0.55mmol)於環戊基甲醚(0.55ml)中之溶液逐滴處理。使反應物經35分鐘溫至-10℃,隨後藉由添加1M氯化銨水溶液(1.4ml)中止。在溫至室溫後,使反應混合物分配於乙酸乙酯(10ml)與水(15ml)之間。
有機相以飽和氯化鈉水溶液(15ml)洗滌;隨後經硫酸鈉脫水;過濾且在真空中蒸發,得到2-(3-戊基苯基)-1,3-二氧雜環戊烷-2-甲酸乙酯(0.1g,60%)。1H NMR(400MHz,CDCl3):δ 7.37-7.43(m,2H),7.10-7.30(m,2H),3.95-4.22(m,6H),2.52-2.62(m,2H),1.52-1.64(m,2H),1.28-1.39(m,4H),1.18-1.26(m,3H),0.79-0.93(m,3H)。
步驟4
2-(3-戊基苯基)-1,3-二氧雜環戊烷-2-甲酸乙酯(0.09g,0.3mmol)於三氟乙酸(2ml)及水(2ml)中之溶液在室溫下攪拌隔夜。用水(20ml)及乙酸乙酯(40ml)稀釋反應混合物,且藉由逐漸添加固體碳酸氫鈉(3.0g)將水相之pH調節至pH 7。有機相隨後經硫酸鈉脫水;過濾且在真空中蒸發,得到粗產物。利用以含0-3%乙酸乙酯之己烷洗提之BiotageTM SP1系統(25g二氧化矽濾筒)純化,得到2-側氧基-2-(3-戊基苯基)乙酸乙酯(8mg,10%)。1H NMR(400MHz,CDCl3):δ 7.71-7.75(m,2H),7.41(d,J=7.6Hz,1H),7.35(dd,J=8.0,7.6Hz,1H),4.39(q,J=7.2Hz,2H),2.60(t,J=7.8Hz,2H),1.53-1.60(m,2H),1.36(t,J=7.2Hz,3H),1.23-1.30(m,4H),0.82(t,J=7.1Hz,3H)。
步驟5
用50mg/ml氫氧化鋰水溶液(0.15ml,0.3mmol)處理2-側氧基-2-(3-戊基苯基)乙酸乙酯(8mg,0.03mmol)於乙腈(0.6ml)中之溶液且反應物在室溫下攪拌隔夜。反應混合物以1M鹽酸水溶液(10ml)中止,且用乙酸乙酯(10ml)萃取。有機相隨後以飽和氯化鈉水溶液(10ml)洗滌;經硫酸鈉脫水;過濾且在真空中蒸發,得到2-側氧基-2-(3-戊基苯基)
乙酸(5.8mg,83%)。1H NMR(400MHz,CDCl3):δ 8.17(d,J=7.6Hz,2H),8.11(s,1H),7.46(d,J=7.6Hz,1H),7.38(dd,J=7.6,7.6Hz,1H),2.61(t,J=7.7Hz,2H),1.62-1.67(m,2H),1.30-1.37(m,4H),0.83(t,J=6.9Hz,3H)。
步驟6
用10mg/ml碳酸氫鈉水溶液(0.19ml,0.02mmol)處理2-側氧基-2-(3-戊基苯基)乙酸(6mg,0.02mmol)於乙醇(0.4ml)中之溶液,且反應物在室溫下攪拌隔夜。在真空中蒸發反應混合物,且將殘餘物溶解于水(1ml)中;過濾(0.2微米);且凍幹,得到2-側氧基-2-(3-戊基苯基)乙酸鈉(3.5mg,58%)。1H NMR(400MHz,CD3OD):δ 7.77-7.79(m,2H),7.38-7.45(m,2H),2.67(t,J=7.7Hz,2H),1.60-1.68(m,2H),1.28-1.39(m,4H),0.90(t,J=7.0Hz,3H);13C NMR(101MHz,CD3OD):δ 196.04,172.87,143.53,133.78,133.76,129.28,128.43,126.94,35.44,31.32,31.06,22.37,13.16;LRMS(ESI負模式):m/z 218.8(100%,M-Na+);UPLC(系統B):4.7分鐘。UPLC系統B:移動相A=0.1%甲酸水溶液;移動相B=含0.1%甲酸之乙腈;固定相=HSS T3管柱;梯度=含5-100% B之A,經10分鐘。
實施例19:
化合物XIX;2-(2-羥基-3-戊基苯基)乙酸之鈉鹽
步驟1
用硫酸(0.95ml,17.8mmol)處理2-(2-羥基苯基)乙酸(3.00g,19.7mmol)於甲醇(40ml)中之溶液,且反應物在室溫下攪拌18小時。用乙酸乙酯(250ml)稀釋反應混合物,且溶液以水(2×150ml)及飽和氯化鈉水溶液(150ml)洗滌;經硫酸鈉脫水;過濾且在真空中蒸發,得到粗產物。自熱己烷中再結晶,得到2-(2-羥基苯基)乙酸甲酯(2.83g,87%)。1H NMR(400MHz,CDCl3):δ 7.20(ddd,J=7.7,7.4,1.8Hz,1H),7.09-7.11(m,1H),6.94(dd,J=8.0,1.2Hz,1H),6.88(ddd,J=7.4,7.4,1.2Hz,1H),3.75(s,3H),3.69(s,2H)。
步驟2
在氮氣下將2-(2-羥基苯基)乙酸甲酯(1.00g,6.0mmol)、三苯基膦(2.37g,9.0mmol)及戊-1-烯-3-醇(0.78g,9.0mmol)於四氫呋喃(30ml)中之溶液冷卻至0℃,且經10分鐘逐滴添加偶氮二甲酸二異丙酯(1.86ml;9.0ml)。隨後將反應物加熱至60℃持續21.5小時。在真空中蒸發溶劑且用含5%乙酸乙酯之己烷萃取殘餘物。過濾萃取物且在真空中蒸發,得到粗產物。利用以含0-3%乙酸乙酯之己烷洗提之BiotageTM SP1
系統(120g二氧化矽濾筒)純化,得到2-(2-(戊-1-烯-3-基氧基)苯基)乙酸甲酯(0.39g,28%)。1H NMR(400MHz,CDCl3):δ 7.21-7.26(m,1H),7.20(d,J=7.6Hz,1H),6.91(ddd,J=7.4,7.4,1.0Hz,1H),6.87(d,J=8.0Hz,1H),5.84(ddd,J=17.4,10.7,6.0Hz,1H),5.26(d,J=17.4Hz,1H),5.22(d,J=10.7Hz,1H),4.63(dt,J=6.0,6.0Hz,2H),3.70(s,3H),3.68(s,2H),1.71-1.87(m,2H),1.02(t,J=7.5Hz,3H);13C NMR(101MHz,CDCl3):δ 172.58,.156.28,137.75,131.19,128.50,123.87,120.52,116.66,113.18,79.76,52.00,36.61,28.71,9.62。
步驟3
在Biotage啟動器中在180℃下用微波輻射照射2-(2-(戊-1-烯-3-基氧基)苯基)乙酸甲酯(0.24g,1.0mmol)於N-甲基-2-吡咯啶酮(1.0ml)中之溶液30分鐘,隨後照射15分鐘。溶液以乙酸乙酯(25ml)稀釋,隨後用水(4×25ml)及飽和氯化鈉水溶液(25ml)洗滌;經硫酸鈉脫水;過濾且在真空中蒸發,得到粗產物。利用以含0-7%乙酸乙酯之己烷洗提之BiotageTM SP1系統(40g二氧化矽濾筒)純化,得到(E)-2-(2-羥基-3-(戊-2-烯基)苯基)乙酸甲酯(0.89g,37%)。1H NMR(400MHz,CDCl3):δ 7.09(s,1H),7.08(dd,J=7.4,1.6Hz,1H),7.01(dd,J=7.6,1.6Hz,1H),6.85(dd,J=7.6,7.4Hz,1H),5.59-5.70(m,2H),3.75(s,3H),3.69(s,2H),3.41(d,J=4.7Hz,2H),2.04-2.11(m,2H),1.01(t,J=7.4Hz,3H);13C NMR(101MHz,CDCl3):δ 174.31,153.53,134.44,129.86,129.32,128.62,127.13,121.08,120.82,52.79,37.59,34.17,25.77,13.97。
步驟4
如化合物I步驟3所述但使用甲醇作為溶劑將(E)-2-(2-羥基
-3-(戊-2-烯基)苯基)乙酸甲酯(0.14g,0.6mmol)氫化,得到2-(2-羥基-3-戊基苯基)乙酸甲酯(0.11g,76%)。1H NMR(400MHz,CDCl3):δ 7.57(s,1H),7.11(dd,J=7.4,1.6Hz,1H),6.96(dd,J=7.4,1.6Hz,1H),6.84(dd,J=7.4,7.4Hz,1H),3.76(s,3H),3.70(s,2H),2.68(t,J=7.8Hz,2H),1.61-1.67(m,2H),1.36-1.43(m,4H),0.93(t,J=7.0Hz,3H);13C NMR(101MHz,CDCl3):δ 175.01,153.48,131.75,129.98,128.75,120.74,120.60,53.01,38.30,32.10,30.50,29.91,22.87,14.34。
步驟5
如化合物I步驟4所述使用乙腈/水(4:1)作為溶劑將2-(2-羥基-3-戊基苯基)乙酸甲酯(0.11g,0.5mmol)水解,得到2-(2-羥基-3-戊基苯基)乙酸(0.57g,57%)。1H NMR(400MHz,CDCl3):δ 8.70(br s,1H),7.09(dd,J=7.6,1.6Hz,1H),6.98(dd,J=7.4,1.6Hz,1H),6.84(dd,J=7.6,7.4Hz,1H),3.68(s,2H),2.62(t,J=7.8Hz,2H),1.57-1.65(m,2H),1.31-1.40(m,4H),0.91(t,J=7.0Hz,3H);13C NMR(101MHz,CDCl3):δ 179.89,152.79,130.92,130.04,128.98,121.08,120.24,37.74,32.02,30.34,29.78,22.80,14.30。
步驟6
如化合物I步驟5所述將2-(2-羥基-3-戊基苯基)乙酸(22mg,0.098mmol)轉化為鈉鹽,得到2-(2-羥基-3-戊基苯基)乙酸鈉(24mg,98%)。1H NMR(400MHz,CD3OD):δ 6.91(dd,J=7.5,1.6Hz,1H),6.87(dd,J=7.5,1.6Hz,1H),6.66(dd,J=7.5,7.5Hz,1H),3.49(s,2H),2.59(t,J=7.7Hz,2H),1.55-1.62(m,2H),1.28-1.38(m,4H),0.90(t,J=7.0Hz,3H);13C NMR(101MHz,CD3OD):δ 180.26,154.27,130.75,128.21,127.90,124.24,119.23,42.91,31.83,30.21,29.82,22.51,13.29;LRMS(ESI負模式):m/z
220.8(100%,M-Na+);UPLC(系統A):5.0分鐘。UPLC系統A:移動相A=10mM甲酸銨水溶液;移動相B=乙腈;固定相=HSS T3管柱;梯度=含5-100% B之A,經10分鐘。
實施例20:
化合物XX;2-(2-苄基-3-羥基-5-戊基苯基)乙酸之鈉鹽
如實施例2(關於化合物XI)所述自(E)-2-(2-苄基-3-(苄氧基)-5-(戊-1-烯基)苯基)乙酸甲酯製備上述化合物。1H NMR(400MHz,CD3OD):δ 7.13-7.18(m,4H),7.03-7.09(m,1H),6.63(d,J=1.6Hz,1H),6.57(d,J=1.6Hz,1H),4.07(s,2H),3.37(s,2H),2.48(t,J=7.7Hz,2H),1.56-1.64(m,2H),1.28-1.39(m,4H),0.90(t,J=6.9Hz,3H);13C NMR(101MHz,CD3OD):δ 179.51,155.24,141.67,141.46,138.05,128.22,127.83,125.14,123.51,121.79,113.06,42.65,35.61,31.66,31.13,31.10,22.49,13.33;LRMS(ESI+):m/z 312.9(90%,M-Na++2H+);UPLC(系統A):6.0分鐘。UPLC系統A:移動相A=10mM甲酸銨水溶液;移動相B=乙腈;固定相=HSS T3管柱;梯度=含5-100% B之A,經10分鐘。
實施例21:
化合物I對博萊黴素誘發之肺纖維化小鼠模型的影響
向小鼠中氣管內滴注抗癌藥物博萊黴素導致急性炎症,接著為慢性纖維變性反應。因此,可藉由在適當時間點處理小鼠來進行諸如化合物I之候選抗纖維變性藥物的評估,且可使用組織學、生物化學及細胞讀數來監測此模型中之候選藥物功效。
雄性C57BL6小鼠於第0天經氣管內滴注投予硫酸博萊黴素(0.025U),隨機分組且於第7天至第20天經投予化合物I(經口投予,100mg/kg及200mg/kg)。
氣管內滴注博萊黴素自第5天至第21天誘發顯著的體重減輕。用200mg/kg化合物I經口處理降低此體重減輕(圖1)。
對此等動物之肺的組織學檢查揭示引人關注的差異。如圖2中所示,經化合物I處理之動物之肺顯示顯著的病變減少。使用HEP(Hemalun與曙紅/玫瑰紅)及Masson三色染色評估病變評分。病變評分記錄為:1)如由破壞之肺結構(蜂巢及/或纖維化)所示之硬結;及2)如由硬結區域之厚度及其外部收縮所示的肺泡壁。用化合物I處理以劑量依賴性方式減少組織學病變。
圖3呈現由博萊黴素誘發之肺纖維化之肺組織的顯微照片。顯而易見,用化合物I處理減少肺中之病變及纖維化。
對肺組織進行進一步分析。藉由即時PCR定量CTGF、膠原1及IL-23p19 mRNA表現。吾等結果顯示,經口投予化合物I顯著降低此等炎性及纖維變性標誌物於肺中之表現,如圖4、圖5及圖6中分別所示。
總之,吾等結果表明,用化合物I處理可有益於預防由臨床使用抗癌化學治療劑諸如博萊黴素所產生之肺損傷的進展或誘導其衰退。此外,吾等結果表明,用化合物I處理可有益於預防肺纖維化(包括特發性肺纖維化(IPF))之進展或對其進行治療。
實施例22:
化合物I及吡非尼酮對博萊黴素誘發之肺纖維化小鼠模型的影響
吡非尼酮在臨床試驗中顯示用於治療IPF之充分藥物功效
從而獲得歐洲及加拿大的批准。因此,藉由上文實施例4中所述相同方案在博萊黴素誘發之肺纖維化小鼠模型中將其與化合物I並行評估。化合物I(200mg/kg)及吡非尼酮(400mg/kg)係單獨或組合經口投予。
將化合物I及吡非尼酮溶解於PBS中。在組合療法中,將吡非尼酮溶解於化合物I之溶液中。用化合物I處理未報導毒性。用吡非尼酮處理誘發嚴重眩暈,其在組合療法中降低(表1)。
對此等動物之肺的組織學檢查揭示引人關注的差異。如圖7中所示,在經化合物I及組合療法(化合物I與吡非尼酮)處理之動物中,受博萊黴素影響之肺的百分比較低。
使用HEP(Hemalun與曙紅/玫瑰紅)及Masson三色染色評估病變評分且記錄為:1)如由破壞之肺結構(蜂巢及/或纖維化)所示之硬結;及2)如由硬結區域之厚度及其外部收縮所示的肺泡壁。如圖8中所呈現,與在組織學水準上顯示纖維化無減少的吡非尼酮相比,用化合物I處理顯著減少組織學病變。化合物I與吡非尼酮之組合進一步減少組織學病變。
藉由使用Masson三色染色之組織形態測量術定量如由白血球浸潤百分比(炎性區域)乘以白血球浸潤物中存在之膠原百分比所測定的病變評分。博萊黴素誘導白血球浸潤中之膠原百分比強烈增加且藉由用化合物I經口處理使其顯著降低,如圖9所示。
圖10呈現用HEP染色之經博萊黴素誘發之肺纖維化的肺組織的顯微照片。顯而易見,如由破壞之肺結構及肺泡壁之間質厚度以及細胞浸潤的減小所觀測,用化合物I處理減少肺中之病變及纖維化。單獨的吡非尼酮無作用。
亦根據Ashcroft評分確定肺纖維化之目測等級。簡言之,由
不知情檢查者觀察每個肺切片之全部區域,且每個區域經目測評定為0至8。用於評定肺纖維化之準則如下:0級=正常肺;1級=肺泡或細支氣管壁之纖維化增厚程度最小;3級=壁增厚程度適中,對肺結構無明顯損傷;5級=纖維化增加,對肺結構有明確損傷,且形成纖維帶或小的纖維塊;7級=結構嚴重變形,且有大的纖維區;8級=肺區域完全被纖維阻塞。
Masson染色顯示肺泡空間加寬且為膠原纖維所填充,指示博萊黴素誘發之肺纖維化中之增殖性纖維母細胞病變(圖11)藉由用化合物I或化合物I與吡非尼酮之組合經口處理而減少。當根據Ashcroft法評級時,單獨的吡非尼酮顯示弱活性。
IPF為一種可導致末期纖維化之慢性間質性肺病。鹹信發病機制與炎性細胞與結構細胞之間的串擾失調有關,由負責維持組織恒定及協調對損傷之反應的各種細胞介素、化學因子及生長因子介導。在所測試之許多細胞介素中,IL-1-β、IL-17及IL-23表明顯著的炎症、組織損傷及慢性纖維化;腫瘤壞死因子-α(TNF-α)及IL-6誘發炎症及輕度纖維化;IL-4及IL-13促進纖維細胞分化及纖維化;TGF-β及CTGF造成輕微炎症,但進行性慢性纖維化顯著。實際上,轉化生長因子(TGF)-β1為肺纖維化發病機制中所涉及之主要促纖維化細胞介素之一。其誘導纖維母細胞分化為肌纖維母細胞,該等肌纖維母細胞產生高含量膠原且伴隨著肺彈性損失及呼吸功能降低。
為測定化合物I對肺纖維化之作用,對肺組織進行進一步分析。藉由即時PCR定量TGF-β、CTGF、IL-23及IL-6 mRNA表現。吾等結果顯示,經口投予化合物I及組合療法顯著降低此等炎性及纖維變性標誌物於肺中之表現,如圖12、圖13、圖14及圖15中分別所示。經口投予吡非尼酮對CTGF mRNA表現無影響,但降低TGF-β、IL-23及IL-6 mRNA表現。
IPF之特徵為纖維母細胞增殖加劇以及膠原及纖維結合蛋白之積聚。改變之纖維結合蛋白表現、降解及組織化與肺纖維化有關。吾等結果顯示,博萊黴素之氣管內吸入增加膠原1與纖維結合蛋白(FN-1)mRNA表現。用化合物I、吡非尼酮及組合療法經口處理誘導此兩種纖維變
性標誌物顯著降至對照水準(圖16及圖17)。另外,用化合物I處理誘導膠原3 mRNA表現的降低較弱,而吡非尼酮處理無影響。然而,組合療法顯著抑制膠原3表現,使其接近於對照水準(圖18)。
實施例23:
化合物I對CCl
4
誘發之肝纖維化小鼠模型的影響
肝纖維化為包括B型肝炎病毒、C型肝炎病毒、酒精性肝病、非酒精性脂肪肝炎及多種慢性中毒之許多慢性肝病的結果。因此需要評估化合物I對鼠科動物CCl4誘發之肝纖維化的影響。CCl4中毒導致肝細胞損傷、壞死、炎症及纖維化,其擴展至與饋入及排出肝竇狀隙之血管結構(分別為肝門通道及中央根靜脈)有關聯,且經8-30周導致纖維化發展為肝細胞癌。因此,可藉由在適當時間點處理小鼠來進行諸如化合物I之候選抗纖維變性藥物之評估,且可使用組織學、生物化學及細胞讀數來監測此模型中之候選藥物功效。
在雄性C57BL/6中每週兩次經腹膜內注射CCl4(10%於玉米油中,2ml/kg),持續16周。自第1天至第113天,每天經口投予化合物I(200mg/kg)。對小鼠實施安樂死且分析組織學及肝纖維變性標誌物。
為測定化合物I是否對肝纖維化有影響,使用羥脯胺酸含量來量測組織中之膠原含量,該膠原含量指示肝纖維化。用化合物I經口處理誘導肝臟中之羥脯胺酸含量顯著降低(圖19)。
使用Masson三色染色在組織學顯微照片中亦觀測到肝組織中膠原含量之降低。圖20中,化合物I誘導膠原評分顯著降低。
Masson三色染色將細胞質、角蛋白、肌纖維及細胞內纖維染成紅色;將細胞核染成黑色且將膠原(纖維組織)染成藍色。如圖21中所示,所有對照小鼠皆揭示膠原之正常分佈。在CCl4誘導之動物中顯而易見大量膠原沈積及橋接纖維化,而在經化合物I處理之動物中觀測到膠原沈積顯著降低且在肝門管-中央管之肝門-肝門之間形成橋接。
用化合物1及化合物V進行另一實驗,其中每週兩次經腹膜內注射CCl4(10%於橄欖油中,2ml/kg)於雄性C57BL/6中,持續8周。
自第1天至第58天每天經口投予化合物1及化合物V(100mg/kg及200mg/kg)。對小鼠實施安樂死且藉由使用Masson三色染色之組織形態量測術定量肝臟中之膠原含量(纖維化標誌物)。用化合物1及化合物V經口處理誘導肝臟中之膠原含量顯著降低(圖22)。
實施例24:
化合物對皮膚纖維化之抗纖維變性作用
使用正常人類皮膚纖維母細胞(NHDF)研究本發明化合物對皮膚纖維化之作用。
進行試管內分析以測定化合物I對正常人類皮膚纖維母細胞(NHDF)上之TGF-β誘導之CTGF、膠原1及α-SMA(纖維化標誌物)的作用。藉由定量即時PCR測定促纖維變性(CTGF)及纖維變性標誌物(膠原1及α-SMA)之表現。如圖23、圖24及圖25中所示,TGF-β(5ng/ml)誘導CTGF、膠原1及α-SMA轉錄物表現的上調,其受化合物I(500μM)抑制。此外,用單獨的化合物I處理細胞導致CTGF、膠原1及α-SMA之基本表現降低。
肌纖維母細胞為源自纖維母細胞、上皮細胞及間質幹細胞/基質細胞(纖維細胞)之最終分化細胞,其經由基質合成(諸如膠原)增加在組織纖維化中起重要作用。α-SMA為肌纖維母細胞之熟知標誌物。吾等結果指示化合物I抑制纖維母細胞分化,如由TGF-β誘導之纖維母細胞中α-SMA受到90%抑制所示。
肌纖維母細胞亦展現增強之遷移表现型(Suganuma等人,1995)且能夠釋放眾多促纖維變性介體。設計後續實驗(刮痕檢定、侵襲/遷移)來測定化合物I對EGF刺激之正常人類皮膚纖維母細胞(NHDF)的作用。總之,用EGF刺激經絲裂黴素處理之NHDF且在化合物I(0.5mM)存在或不存在(對照物)下進行培育。EGF刺激纖維母細胞侵入刮痕中,其受到化合物I抑制(圖26)。
實施例25:
化合物對纖維母細胞及上皮細胞之纖維變性標誌物的抗纖維變性作用
CTGF、膠原1及α-SMA為由活化纖維母細胞及經歷上皮-間質轉化(EMT)之上皮細胞產生的纖維變性標誌物。使用TGF-β來誘導HK-2細胞(上皮細胞)中之EMT以及誘導活化之纖維母細胞(正常人類皮膚纖維母細胞(NHDF)及大鼠纖維母細胞(NRK-49F))來分泌膠原且強烈表現α-SMA。藉由定量即時PCR測定纖維變性標誌物(膠原1及α-SMA)之表現。如表2中所示,在上皮細胞及纖維母細胞中本發明化合物抑制膠原1及α-SMA。
表2:已針對根據本發明之若干化合物測定上皮細胞(HK2細胞)及纖維母細胞(NHDF)中膠原之抑制百分比及纖維母細胞(NRK-49F及NHDF)中α-SMA之抑制百分比。在所有情況下,已量測膠原及α-SMA之mRNA,且在相應濃度之測試化合物存在下評估抑制作用。已在不同濃度[mM]下測試該等化合物。所有化合物皆降低HK-2、NHDF及NRK-49F細胞中膠原及α-SMA之表現。
n.d.意謂未測定
實施例26:化合物I對小鼠模型中心臟纖維化之作用
在5/6腎切除(5/6-Nx)模型中植入股動脈導管使心臟纖維化之存在增加且使用其來評估化合物I對心臟纖維化之作用。總而言之,使雄性6周齡Sprague-Dawley大鼠進行5/6-Nx或假操作。簡言之,在第0天移除三分之二的左腎,接著在第7天進行右腎完全切除。在第7天經由股靜脈植入導管。使假操作大鼠之腎臟暴露且移除腎周脂肪並用作對照。用媒劑(水)處理經歷假操作之動物且用作對照。在第21天,基於大鼠之腎小球濾過率(GFR)結果將其隨機分組。藉由每週三次經靜脈內投予化合物I(10mg/kg)或每天經口投予化合物I(200mg/kg)來處理5/6-Nx動物。藉由量測羥脯胺酸(膠原含量)及組織學評估(HPE及Masson三色染色)來測定心臟纖維化。
如所述,相比於經口處理(無導管),在經插入導管之5/6腎切除動物中植入導管以供靜脈內投予化合物誘發心臟纖維化。經口處理在本文與措辭「po」相同,意謂「經口」;靜脈內投予與措辭「iv」相同,意謂「靜脈內」。如圖27中所例示,5/6-Nx大鼠具有弱的心臟病變。然而,植入導管誘導心臟病變(纖維化、壞死及炎症)顯著增加(4倍)。
如圖28中所示,可見用靜脈內化合物I處理顯著(p<0.05)減少總心臟病變,其包括如圖29中所報導之炎症顯著減少及如圖30中所報導之壞死顯著減少。
進行進一步分析以藉由量測羥脯胺酸(其于膠原中特異性檢測)來測定心臟膠原含量。在腎切除大鼠之心臟中,羥脯胺酸含量(膠原)顯著增加,如圖31中所報導。用化合物I經靜脈內處理及經口處理皆誘導羥脯胺酸含量顯著降低(圖30)。
此種羥脯胺酸(膠原)含量降低與用Masson三色染色(其用於染色膠原(藍))之心臟的組織學顯微照片相關。圖32及圖33分別展示代表性動物之心臟的40倍及100倍放大視圖顯微照片,其中化合物I係經口投予,與未接受化合物I之腎切除動物進行比較。圖34展示代表性動物之心臟的40倍放大視圖顯微照片,其中化合物I係經靜脈內投予,與未接受化合物I之腎切除動物進行比較。圖32、圖33及圖34為動物之心臟的顯微照片,其顯示類似的血清肌酐含量。在所有顯微照片中,顯而易見,用化合物I經靜脈內處理及經口處理可減少纖維化(藍色膠原沈積)。
本文提及或引用之所有專利、專利申請案、臨時申請案及公開案皆以全文引用之方式併入,包括所有圖式及表格,引用程度使得其與本說明書之明確教示不一致。
應理解,本文所述之實施例及實施方案僅為說明性目的且根據其之各種修改或變化應為熟習此項技術者所想到且包括於本申請案之精神及範圍內。
Claims (18)
- 一種由下式表示之化合物或其醫藥學上可接受之鹽於製造藥物上的用途,該藥物是用於在患有纖維變性疾病之個體中減緩纖維化之進展及/或治療纖維化,其中該纖維變性疾病為皮膚纖維化或心臟纖維化,且其中該皮膚纖維化為瘢痕形成、增生性瘢痕形成、瘢痕瘤及皮膚纖維變性病症,且其中該心臟纖維化為心肌病:其中A為C5烷基、C6烷基、C5烯基、C6烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為3或4;R1為H、OH或F;R2為H、OH、F或CH2-OH;R3為H、OH、F或CH2Ph;R4為H、OH或F;Q為1)(CH2)mC(O)OH,其中m為1或2,2)CH(F)-C(O)OH,3)CF2-C(O)OH,或4)C(O)-C(O)OH。
- 如請求項1之用途,其中該化合物之醫藥學上可接受之鹽為鈉鹽、鉀 鹽、鋰鹽、銨鹽、鈣鹽、鎂鹽、錳鹽、鋅鹽、鐵鹽或銅鹽。
- 如請求項2之用途,其中該化合物之醫藥學上可接受之鹽為鈉鹽。
- 如請求項4之用途,其中該化合物為化合物I。
- 如請求項4之用途,其中該化合物為化合物V。
- 如請求項1至6中任一項之用途,其中該纖維變性疾病為皮膚纖維化。
- 如請求項7之用途,其中該皮膚纖維化為瘢痕形成。
- 如請求項8之用途,其中該瘢痕形成源自傷口、燒傷、瘢痕、皺紋、妊娠紋、曬傷、化學損傷、熱損傷、冷損傷、創傷、手術損傷、輻射或潰瘍。
- 如請求項9之用途,其中該潰瘍為糖尿病性足潰瘍、靜脈性腿潰瘍或壓力性潰瘍。
- 如請求項7之用途,其中該化合物或其醫藥學上可接受之鹽是以治療有效量來使用,該治療有效量為介於約1至約50mg/kg之間,該化合物係經口投予,且該個體為人類。
- 如請求項7之用途,其中該化合物或其醫藥學上可接受之鹽係用於經局部投予。
- 如請求項12之用途,其中該個體為人類,且其中該化合物或其醫藥學上可接受之鹽是以約0.01%至約10%(w/w)的劑量來使用。
- 如請求項1至6中任一項之用途,其中該纖維變性疾病為心臟纖維化。
- 如請求項14之用途,其中該化合物或其醫藥學上可接受之鹽是以治療有效量來使用,該治療有效量為介於約1至約50mg/kg之間,該化合物係經口投予,且該個體為人類。
- 如請求項1至15中任一項之用途,其中該化合物或其醫藥學上可接受之鹽與治療有效量之第二化合物組合使用,該第二化合物為免疫抑制藥物、消炎藥物、細胞介素、單株抗體、多重受體酪胺酸激酶抑制劑、抗氧化劑、酶抑制劑、整合素抑制劑、脂質受體調節劑或噻唑啉二酮。
- 一種用於在有需要之個體中預防纖維變性疾病及/或減緩纖維變性疾病之進展及/或治療纖維變性疾病的套組,其包含由下式表示之化合物:或其醫藥學上可接受之鹽,其中A為C5烷基、C6烷基、C5烯基、C6烯基、C(O)-(CH2)n-CH3或CH(OH)-(CH2)n-CH3,其中n為3或4;R1為H、OH或F;R2為H、OH、F或CH2-OH;R3為H、OH、F或CH2Ph;R4為H、OH或F;Q為1)(CH2)mC(O)OH,其中m為1或2,2)CH(F)-C(O)OH,3)CF2-C(O)OH,或4)C(O)-C(O)OH;以及關於向罹患該纖維變性疾病之該個體投予治療有效量之該化合物的說明書,其中該纖維變性疾病為皮膚纖維化或心臟纖維化,其中該皮膚纖維化為瘢痕形成、增生性瘢痕形成、瘢痕瘤及皮膚纖維變性病症,且其中該心臟纖維化為心肌病。
- 如請求項17之套組,其進一步包含關於向人類個體每天經口投予介於約1至約50mg/kg之間之該化合物的說明書。
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ITMI20012434A1 (it) * | 2001-11-20 | 2003-05-20 | Dompe Spa | Acidi 2-aril-propionici e composizioni farmaceutiche che li contengono |
SG175855A1 (en) * | 2009-05-04 | 2011-12-29 | Prometic Biosciences Inc | Substituted aromatic compounds and pharmaceutical uses thereof |
JP5844251B2 (ja) | 2009-05-04 | 2016-01-13 | プロメティック・バイオサイエンシーズ・インコーポレイテッドProMetic BioSciences Inc. | 3−ペンチルフェニル酢酸の塩およびその薬学的使用 |
US9114118B2 (en) * | 2010-10-27 | 2015-08-25 | Prometic Biosciences Inc. | Compounds and compositions for the treatment of cancer |
CN102070433B (zh) * | 2010-12-27 | 2013-03-27 | 桂林师范高等专科学校 | 芳香基乙酸类衍生物的制备方法 |
TWI742541B (zh) * | 2013-03-15 | 2021-10-11 | 英商邊緣生物科技有限公司 | 用於治療肺纖維化、肝纖維化、皮膚纖維化及心臟纖維化之經取代之芳族化合物 |
TWI689490B (zh) * | 2013-03-15 | 2020-04-01 | 英商邊緣生物科技有限公司 | 用於治療纖維化之經取代之芳族化合物及相關方法 |
RU2728782C2 (ru) * | 2014-11-12 | 2020-07-31 | Лиминал Байосайенсиз Лимитед | Замещенные ароматические соединения и фармацевтические композиции для ауторепарации и регенерации ткани |
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